EP3512881A1 - Treatment of non-hodgkin lymphoma using lilotomab and 177lu-lilotomab satetraxetan - Google Patents

Treatment of non-hodgkin lymphoma using lilotomab and 177lu-lilotomab satetraxetan

Info

Publication number
EP3512881A1
EP3512881A1 EP17768448.7A EP17768448A EP3512881A1 EP 3512881 A1 EP3512881 A1 EP 3512881A1 EP 17768448 A EP17768448 A EP 17768448A EP 3512881 A1 EP3512881 A1 EP 3512881A1
Authority
EP
European Patent Office
Prior art keywords
lilotomab
satetraxetan
lilotomab satetraxetan
administered
treatment
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Pending
Application number
EP17768448.7A
Other languages
German (de)
French (fr)
Inventor
Jostein Dahle
Simon Turner
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Thor Medical ASA
Original Assignee
Nordic Nanovector AS
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Nordic Nanovector AS filed Critical Nordic Nanovector AS
Publication of EP3512881A1 publication Critical patent/EP3512881A1/en
Pending legal-status Critical Current

Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K51/00Preparations containing radioactive substances for use in therapy or testing in vivo
    • A61K51/02Preparations containing radioactive substances for use in therapy or testing in vivo characterised by the carrier, i.e. characterised by the agent or material covalently linked or complexing the radioactive nucleus
    • A61K51/04Organic compounds
    • A61K51/0474Organic compounds complexes or complex-forming compounds, i.e. wherein a radioactive metal (e.g. 111In3+) is complexed or chelated by, e.g. a N2S2, N3S, NS3, N4 chelating group
    • A61K51/0482Organic compounds complexes or complex-forming compounds, i.e. wherein a radioactive metal (e.g. 111In3+) is complexed or chelated by, e.g. a N2S2, N3S, NS3, N4 chelating group chelates from cyclic ligands, e.g. DOTA
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K51/00Preparations containing radioactive substances for use in therapy or testing in vivo
    • A61K51/02Preparations containing radioactive substances for use in therapy or testing in vivo characterised by the carrier, i.e. characterised by the agent or material covalently linked or complexing the radioactive nucleus
    • A61K51/04Organic compounds
    • A61K51/08Peptides, e.g. proteins, carriers being peptides, polyamino acids, proteins
    • A61K51/10Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody
    • A61K51/1027Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody against receptors, cell-surface antigens or cell-surface determinants
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K51/00Preparations containing radioactive substances for use in therapy or testing in vivo
    • A61K51/02Preparations containing radioactive substances for use in therapy or testing in vivo characterised by the carrier, i.e. characterised by the agent or material covalently linked or complexing the radioactive nucleus
    • A61K51/04Organic compounds
    • A61K51/08Peptides, e.g. proteins, carriers being peptides, polyamino acids, proteins
    • A61K51/10Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody
    • A61K51/1045Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody against animal or human tumor cells or tumor cell determinants
    • A61K51/1069Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody against animal or human tumor cells or tumor cell determinants the tumor cell being from blood cells, e.g. the cancer being a myeloma
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K51/00Preparations containing radioactive substances for use in therapy or testing in vivo
    • A61K51/02Preparations containing radioactive substances for use in therapy or testing in vivo characterised by the carrier, i.e. characterised by the agent or material covalently linked or complexing the radioactive nucleus
    • A61K51/04Organic compounds
    • A61K51/08Peptides, e.g. proteins, carriers being peptides, polyamino acids, proteins
    • A61K51/10Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody
    • A61K51/1093Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody conjugates with carriers being antibodies
    • A61K51/1096Antibodies or immunoglobulins; Fragments thereof, the carrier being an antibody, an immunoglobulin or a fragment thereof, e.g. a camelised human single domain antibody or the Fc fragment of an antibody conjugates with carriers being antibodies radioimmunotoxins, i.e. conjugates being structurally as defined in A61K51/1093, and including a radioactive nucleus for use in radiotherapeutic applications
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • A61P35/02Antineoplastic agents specific for leukemia
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • C07K16/18Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans
    • C07K16/28Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants
    • C07K16/2887Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants against CD20
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • C07K16/18Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans
    • C07K16/28Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants
    • C07K16/2896Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants against molecules with a "CD"-designation, not provided for elsewhere
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07KPEPTIDES
    • C07K16/00Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies
    • C07K16/18Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans
    • C07K16/28Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants
    • C07K16/30Immunoglobulins [IGs], e.g. monoclonal or polyclonal antibodies against material from animals or humans against receptors, cell surface antigens or cell surface determinants from tumour cells
    • C07K16/3061Blood cells
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K39/00Medicinal preparations containing antigens or antibodies
    • A61K2039/505Medicinal preparations containing antigens or antibodies comprising antibodies
    • A61K2039/507Comprising a combination of two or more separate antibodies
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K39/00Medicinal preparations containing antigens or antibodies
    • A61K2039/545Medicinal preparations containing antigens or antibodies characterised by the dose, timing or administration schedule
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K2121/00Preparations for use in therapy

Definitions

  • the invention relates to the use of monoclonal antibodies conjugated with 177 Lu in the treatment of Non-Hodgkin lymphoma. Aspects included specific administration patterns, with specific concentrations, pre-treatments and predosing, wherein 177 Lu- lilotomab satetraxetan is the central medicament.
  • Non-Hodgkin Lymphomas (NHL) as a group is the most common malignant
  • NHLs are a diverse group of blood cancers that include any kind of lymphoma except Hodgkin lymphoma. NHLs are tumours developed from lymphocytes, a type of white blood cells. NHLs vary in their clinical behaviour, morphologic appearance, immunologic and molecular phenotype. The various types represent neoplastic lymphoid cells arrested at different stages of differentiation.
  • NHLs can be clinically classified as indolent, aggressive, and highly aggressive. Diffuse large B-cell and follicular lymphoma are the most common subtypes.
  • NHLs are the fifth most common cause of cancer in the United States, with an estimated incidence of 70,130 cases in 2012. Follicular center cell lymphomas are the second most common subtype, comprising approximately 40% of all NHLs. Since 1950, the incidence of NHL has steadily increased at approximately 4% per year. Treatment usually depends on the type of lymphoma and its stage, as well as other prognostic factors. The different treatment options are radiation therapy,
  • rituximab immunotherapy
  • rituximab immunotherapy
  • chemotherapy or a combination of drugs such as CHOP (cyclophosphamide, hydroxydaunorubicin, Oncovin and prednisone) regimen is used.
  • CHOP cyclophosphamide, hydroxydaunorubicin, Oncovin and prednisone
  • RIT relapsed indolent lymphoma
  • rituximab chemotherapy combined with rituximab or other chemotherapy combinations although the proportion responding decreases with each relapse.
  • the aim of RIT is to use a monoclonal antibody (MoAb) to target an isotope for radiation to tumour tissue while limiting the toxicity to normal cells.
  • Beta-emitting radioimmunoconjugates (RIC) possess high levels of clinical activity in patients with relapsed or refractory B-cell lymphomas, including those refractory to rituximab and chemotherapy.
  • Clinical data have validated that RIT is both more cost effective and more efficacious than nonradioactive immunotherapy. More recently, several single- arm studies have demonstrated that upfront RIT administered either alone or with chemotherapy to previously untreated indolent NHL patients produces overall response rates of 90-100 %, complete response rates of 60-95 % and durable remissions.
  • a phase III study of RIT as part of frontline therapy for indolent NHL reported that consolidation therapy with 90 Y-ibritumomab tiuxetan (Zevalin) after induction chemotherapy markedly prolonged progression free survival in patients with previously untreated stage II or IV follicular lymphoma.
  • Zevalin Y-ibritumomab tiuxetan
  • patients with indolent and aggressive NHLs received four cycles of chemotherapy followed by high myeloablative dose 90 Y-ibritumomab tiuxetan followed by autologous stem cell support. After a follow up time of 30 months, the overall survival rate was 87 % and the event free survival was 69 %.
  • CD37 antibodies were compared with CD20 antibodies and a higher grade of internalization and degradation of 131 I-labeled RIC was found for CD37 than for CD20. Furthermore, a favorable biodistribution was obtained in 59 % of the patients for CD20 and for 50 % of the patients for CD37. The amount of cold priming with antibody necessary to get a favorable biodistribution was higher for CD37 than for CD20.
  • leukemia/lymphoma cell lines and primary chronic lymphocytic leukaemia cells are included in the leukemia/lymphoma cell lines and primary chronic lymphocytic leukaemia cells.
  • Lilotomab and the anti-CD20 antibody rituximab have been labeled with both 125 I and m In and measured cell bound activity after 4 days of incubation with a lymphoma cell line.
  • the results show that the problem of catabolism of RIC can be circumvented by labeling with metallic nuclides such as m In or 177 Lu.
  • Beta particles are electrons emitted from the nucleus of an atom. Beta emitters approved for therapy include
  • Betalutin (lilotomab labeled with 177 Lu via the chelator p-SCN-benzyl-DOTA, or 177 Lu- lilotomab satetraxetan) has been developed by Nordic Nanovector in collaboration with the Norwegian Radium Hospital for the treatment of relapsed NHL.
  • RIT permits delivery of a therapeutic dose of radiation directly to the DNA of tumour cells.
  • the radionuclide 177 Lu is a beta-particle emitter.
  • the beta particles are electrons with energy and range in tissue suitable for treating NHLs.
  • the absorbed radiation results in DNA damage and tumour cell death.
  • the radiation emitted from the radiolabeled antibody affects not only the antibody-binding cell, but also neighbouring cells. This mechanism of action of RIT may be especially beneficial in treating patients with bulky or poorly vascularized tumours.
  • Betalutin has been tested for targeting, therapeutic and toxic effect in cells and in mice. Lilotomab has similar or better binding properties to CD37 as rituximab has to CD20.
  • Betalutin Treatment against single cells showed a significantly better effect of Betalutin than of 177 Lu-rituximab.
  • the MTD of Betalutin in SCID mice with tumour cells in the bone marrow was between 50 and 100 MBq/kg (Dahle et al. 2013). In studies with nude mice without tumour cells in the bone marrow the MTD is above 500 MBq/kg (Repetto et al. 2015).
  • Betalutin has a suitable biodistribution profile with high uptake in tumour cells, and that the efficacy results in the mouse models show promise of potentially interesting clinical results.
  • 177 Lu-lilotomab satetraxetan is a candidate for the treatment of Non-Hodgkin lymphoma.
  • 177 Lu-lilotomab satetraxetan can be used in the general population.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m 2 lilotomab, followed by 10-50 MBq/kg 177 l_u-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising predosing of 20-250 mg/m 2 lilotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of lilotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m 2 lilotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Yet another aspect of the present invention relates to lilotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 20- 250 mg/m 2 .
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of 177 Lu-lilotomab satetraxetan in an administration pattern comprising predosing of 20-250 mg/m 2 lilotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An embodiment of the present invention relates to 177 l_u-lilotomab satetraxetan administered at a concentration selected from the group consisting of 10, 12,5, 15, 17.5, 20, 25, 30, 35, 40, 45 and 50 MBq/kg.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration selected from the group consisting of 20, 40, 50, 60, 75, 100, 125, 150, 200, 250 mg/m 2 .
  • a further embodiment of the present invention relates to the predosing of lilotomab done less than 24 hours, such as within 4 hours, before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more infusions of 375 mg/m 2 rituximab.
  • Yet another embodiment of the present invention relates to 375 mg/m 2 rituximab infused at 28 and 21 days before administration of 177 Lu-lilotomab satetraxetan.
  • a further embodiment of the present invention relates to 375 mg/m 2 rituximab infused at 14 days before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to 375 mg/m 2 rituximab infused at 14 days and within 4 hours before administration of 177 Lu-lilotomab satetraxetan.
  • lymphoma being a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, and mantle cell.
  • Figure 1 shows platelet counts of arm 3 (rituximab predosing) and arm 4 ( 100 mg/m 2 lilotomab predosing).
  • arm 3 rituximab predosing
  • arm 4 100 mg/m 2 lilotomab predosing
  • the patients in arm 3 suffers grade 3-4 hematological toxicity while there is no toxicity in arm 4.
  • Figure 2 shows neutrophil counts of arm 1 (40 mg lilotomab predosing), arm 3 (rituximab predosing) and arm 4 ( 100 mg/m 2 lilotomab predosing).
  • arm 3 40 mg lilotomab predosing
  • arm 4 100 mg/m 2 lilotomab predosing.
  • the patients in arm 3 suffers grade 3-4 toxicity, while there is no toxicity of arm 4 and arm 1 is in between.
  • Figure 3 shows PK profiles that show a large separation between the treatment arms.
  • Arm 1 40 mg lilotomab predosing
  • Arm 2 no predosing
  • Arm 3 rituximab predosing
  • Arm 4 100 mg/m 2 lilotomab predosing.
  • Figure 4 shows an example of an administration pattern.
  • Figure 5 shows platelet counts of patients in arm 1 (40 mg predosing), arm 2 (no predosing), arm 3 (rituximab predosing) and arm 4 (100 mg/m 2 lilotomab predosing). There was grade 3-4 toxicity of arm 2 and 3, less toxicity of arm 1 and no toxicity of arm 4.
  • Figure 6 shows neutrophil counts of patients in arm 1 (40 mg predosing), arm 2 (no predosing), arm 3 (rituximab predosing) and arm 4 (100 mg/m 2 lilotomab predosing). There was grade 3-4 toxicity of arm 2 and 3, less toxicity of arm 1 and no toxicity of arm 4.
  • Figure 7 shows PK profiles that show a large separation between the treatment arms.
  • Arm 1 40 mg lilotomab predosing
  • Arm 2 no predosing
  • Arm 3 rituximab predosing
  • Arm 4 100 mg/m 2 lilotomab predosing.
  • Figure 8 shows examples of an administration patterns tested.
  • Figure 9 shows that the mean values for platelets and neutrophils at nadir for 23 arm 1 patients were lower than the mean values for 3 arm 4 patients.
  • Figure 10 shows dose limiting toxicity and number of grade 3 and 4 adverse events were lower for arm 4 than for arm 1 and highest for arm 2.
  • Figure 11 shows the response rates for each to the tested administration patterns.
  • Figure 12 shows four different combinations of pre-dosing and pre-treatment that have been investigated.
  • Two arms included cold lilotomab pre-dosing (arm 1 and 4; 40 mg fixed and 100 mg/m 2 Body Surface Area dosage, respectively) and two did not (arm 2 and 3).
  • Pre-dosing with lilotomab has a mitigating effect on red marrow absorbed dose for 177 Lu-lilotomab satetraxetan patients, and increased amounts was found correlated with a higher tumour dose.
  • Figure 13 shows mean platelet count in Arms 1 and 4 for 15 and 20 MBq/kg 177 Lu- lilotomab satetraxetan.
  • Figure 14 shows mean neutrophil count in Arms 1 and 4 for 15 and 20 MBq/kg 177 Lu- lilotomab satetraxetan.
  • the present invention relates to the treatment of Non-Hodgkin lymphoma using 177 Lu- lilotomab satetraxetan with lilotomab and with or without rituximab, where the inventors surprisingly have found that a specific treatment pattern have advantageous effects.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma or other CD37 positive blood cancers, wherein 177 Lu-lilotomab satetraxetan is administered according to a clinically relevant administration pattern comprising 10-20 MBq/kg 177 Lu-lilotomab satetraxetan, to a person in need thereof.
  • the clinically relevant administration pattern can be seen as an administration pattern that has clinical relevance and effect on human individuals suffering from Non-Hodgkin lymphoma.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 l_u-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20- 100 mg/m 2 lilotomab, followed by b) 10-20 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • treatment be seen as the partial of full treatment of cancer, including any amelioration and for example stabilization of progressing disease.
  • treatment may be seen as an improvement of any of the criteria tested in the examples of the present disclosure.
  • One criteria is overall response rate (ORR). Another is complete response (CR). A further is partial response (PR). Another is stable disease (SD).
  • the lilotomab predosing effect is likely caused by blocking of the binding on remaining B-cells in the lymphoid organs. This can be more effective after rituximab treatment.
  • Pre-medication consisting of an antipyretic and antihistamine medication can be administered before infusion of lilotomab.
  • an aspect of the present invention relates to 177 Lu-lilotomab satetraxetan and lilotomab for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to a specific administration pattern.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m 2 lilotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • the predosing of 20-250 mg/m 2 lilotomab may be substituted with 40-500 mg/patient in all aspects and embodiments of the invention.
  • a further aspect of the present invention relates to lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising predosing of 20-250 mg/m 2 lilotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of Iiiotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein Iiiotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m 2 Iiiotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Yet another aspect of the present invention relates to Iiiotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan, wherein Iiiotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 20- 250 mg/m 2 .
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of 177 Lu-lilotomab satetraxetan in an administration pattern comprising predosing of 20-250 mg/m 2 Iiiotomab, followed by 10-50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • the therapy or treatment of the present invention can be administered either as a monotherapy or in combination with other therapies, preferentially standard treatments.
  • Such other therapies may be one or more selected from the group consisting of pretreatment, surgery, chemotherapy (including doxorubicin, vinblastin and gemcitabine), immunotherapy, antibody therapy, photodynamic therapy, proteasome inhibitor (including bortezomib), histone deacetylase inhibitors (including vorinostat and suberoylanilide hydroxamic acid), vitamin D3 and vitamin D3 analogs, cell cycle checkpoint inhibitors (including UCN-01 and 2-(4-(4-Chlorophenoxy)phenyl)-lH- benzimidazole-5-carboxamide), hypoxic cell radiosensitizers (including metronidazole and misonidazole), apoptosis inducers (including withaferin A and venetoclax), radiosensitizers, radioimmunotherapy or a combination of two or more of these.
  • chemotherapy including doxorubicin, vinblastin and gemcitabine
  • immunotherapy including antibody therapy, photodynamic therapy, proteasome inhibitor (
  • the present invention has the patient being treated according to the present invention already been undergoing treatment for cancer.
  • this treatment of therapy one or more of those mentioned above.
  • the therapy rituximab is the therapy rituximab, and in this case can the patient be a patient relapsing after rituximab treatment.
  • an embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to the present invention, wherein the patient is relapsing after treatment with rituximab.
  • the monoclonal antibody (mAb or moAb) lilotomab was previously known as tetulomab or HH 1 while 177 Lu-lilotomab satetraxetan was previously known as 177 Lu-labeled HH 1 antibody, or named 177 Lu-tetulomab or by the tradename Betalutin.
  • Lu-lilotomab satetraxetan is a radioimmunoconjugate (RIC) also known as antibody radionuclide conjugate (ARC) that is capable of binding to or targeting an antigen of interest. In the present case is this antigen CD37.
  • RIC radioimmunoconjugate
  • ARC antibody radionuclide conjugate
  • Satetraxetan is a derivative of DOTA, p-SCN-benzyl-DOTA.
  • the radioimmunoconjugate and antibody of the present invention can be administered directly in a vein by a peripheral cannula connected to a drip chamber that prevents air embolism and allows an estimate of flow rate into the patient.
  • the radioimmunoconjugate and/or antibody can be administered in a repeated fashion.
  • radioimmunoconjugate followed by monoclonal antibody (or immunoconjugate) can both be administered in a repeated fashion.
  • An embodiment of the present invention relates to the use of the radioimmunoconjugate and/or antibody of the present invention administered in combination with or in addition to other therapy.
  • the other therapies are selected from pretreatment, chemotherapy, monoclonal antibody therapy, surgery, radiotherapy, and/or photodynamic therapy.
  • the other therapies are bone marrow transplantation or stem cell transplantation and/or therapy.
  • 177 Lu-lilotomab satetraxetan used in the treatment of Non- Hodgkin's lymphoma.
  • An embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration selected from the group consisting of 10, 12,5, 15, 17.5, 20, 25, 30, 35, 40, 45, 50 MBq/kg.
  • An embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 10 MBq/kg.
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 12,5 MBq/kg.
  • a further embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5-20 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 l_u-lilotomab satetraxetan administered at a concentration of 20-25 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 25-30 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 30-35 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 35-40 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 40-45 MBq/kg.
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 45-50 MBq/kg.
  • Lilotomab is used for predosing before administration of 177 Lu-lilotomab satetraxetan.
  • An embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 2-50 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 100 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 120 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 150 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 200 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 20 mg/m 2 .
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/m 2 .
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 60 mg/m 2 .
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 20 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 20 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 20 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/m 2 followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/patient followed by 177 l_u-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 50 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 60 mg/patient followed by 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
  • a further embodiment of the present invention relates to lilotomab administered at a concentration of 50 mg/m 2 . This may in an embodiment of the invention be equal to 100 mg/patient.
  • a further embodiment of the present invention relates to lilotomab administered at a concentration of 60 mg/m 2 . This may in an embodiment of the invention be equal to 120 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 125 mg/m 2 . This may in an embodiment of the invention be equal to 250 mg/patient.
  • a further embodiment of the present invention relates to lilotomab administered at a concentration of 150 mg/m 2 . This may in an embodiment of the invention be equal to 300 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 175 mg/m 2 . This may in an embodiment of the invention be equal to 350 mg/patient.
  • a further embodiment of the present invention relates to lilotomab administered at a concentration of 200 mg/m 2 . This may in an embodiment of the invention be equal to 400 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 225 mg/m 2 . This may in an embodiment of the invention be equal to 450 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 50 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 60 mg/patient.
  • Yet another embodiment of the present invention relates to lilotomab administered at a concentration of 250 mg/m 2 . This may in an embodiment of the invention be equal to 500 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 20-250 mg/m 2 . This may in an embodiment of the invention be equal to 10-125 mg/patient.
  • a further embodiment of the present invention relates to lilotomab administered at a concentration of 20-100 mg/m 2 . This may in an embodiment of the invention be equal to 40-200 mg/patient.
  • Another embodiment of the present invention relates to lilotomab administered at a concentration of 20-150 mg/m 2 . This may in an embodiment of the invention be equal to 40-300 mg/patient.
  • a further embodiment of the present invention relates to lilotomab administered at a concentration of 100-200 mg/m 2 . This may in an embodiment of the invention be equal to 200-400 mg/patient. Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 15-20 MBq/kg and lilotomab administered at a concentration of 20-100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 15-20 MBq/kg and lilotomab administered at a concentration of 40-100 mg/m 2 .
  • This may in an embodiment of the invention be equal to 80-200 mg/patient.
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5-20 MBq/kg and lilotomab administered at a concentration of 40-100 mg/m 2 .
  • a further embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 30 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 35 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 40 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 45 MBq/kg and lilotomab administered at a concentration of 100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 30 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m 2 .
  • a further embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • a further embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 30 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 35 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • a further embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 40 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • Another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 45 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • Yet another embodiment of the present invention relates to 177 Lu-lilotomab satetraxetan administered at a concentration of 50 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m 2 .
  • the PK profiles (e.g. figure 3) show activity in kBq/ml in the hours after 177 Lu-lilotomab satetraxetan administration.
  • a high concentration means that a high amount of 177 Lu- lilotomab satetraxetan is present in the blood.
  • immunosuppressive agents may be associated with the occurrence of hematologic toxicity, such as anemia, due to bone marrow suppression or hemolysis, leukopenia, neutropenia and thrombocytopenia.
  • Neutropenia is graded; grade 1 is Neutrophils ⁇ LLN to 1500/mm 3 , grade 2 is Neutrophils ⁇ 1500/mm 3 to 1000/mm 3 , grade 3 is Neutrophils ⁇ 1000/mm 3 to 500/mm 3 , and grade 4 is Neutrophils ⁇ 500/mm 3 (see also figure 2)
  • Thrombocytopenia is graded; grade 1 is Platelets ⁇ LLN to 75,000/mm 3 , grade 2 is ⁇ 75,000/mm 3 to 50,000/mm 3 , grade 3 is ⁇ 50,000/mm 3 to 25,000/mm 3 , and grade 4 is ⁇ 25,000/mm 3 (see also figure 1).
  • thrombocytopenia grade 4 observed after the treatment, and even more preferably is no grade 3 or 4 observed 45 days after the treatment.
  • neutropenia and thrombocytopenia In one embodiment is no grade 3 or 4 neutropenia and thrombocytopenia or no grade 3 neutropenia and thrombocytopenia observed 45 days after the treatment.
  • Neutropenia and thrombocytopenia in patients can for example be seen in example 1 and figures 1 and 2.
  • An aspect of the present invention relates to the use of lilotomab to reduce hematologic toxicity such as neutropenia and/or thrombocytopenia in patients suffering from non- Hodgkin's lymphoma. These patients may previously be treated with rituximab. The patients may also subsequently be treated with 177 Lu-lilotomab satetraxetan as disclosed herein.
  • radioimmunoconjugates and/or antibody can be used in combination with other types of therapy.
  • a further embodiment of the present invention is the use for a combinational therapy where the radioimmunoconjugate followed by simultaneous or post-treatment with antibody therapy, immunoconjugate therapy or a combination thereof, as described elsewhere herein.
  • Such therapy or treatment may be a monoclonal antibody selected from rituximab and lilotomab (HH 1) depending on the antigen in focus.
  • HH 1 lilotomab
  • the therapy can be repeated in cyclic pattern where administration of the radioimmunoconjugates and the monoclonal antibodies are repeated once, twice or several times.
  • a further embodiment of the present invention relates to the predosing of lilotomab done less than 24 hours, such as within 4 hours before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to the predosing of lilotomab done less than 12 hours before administration of 177 Lu-lilotomab satetraxetan.
  • a further embodiment of the present invention relates to the predosing of lilotomab done less than 8 hours before administration of 177 Lu-lilotomab satetraxetan.
  • Yet another embodiment of the present invention relates to the predosing of lilotomab done less than 4 hours before administration of 177 Lu-lilotomab satetraxetan.
  • a further embodiment of the present invention relates to the predosing of lilotomab done less than 2 hours before administration of 177 Lu-lilotomab satetraxetan.
  • Rituximab is a monoclonal antibody against the protein CD20, which is primarily found on the surface of immune system B cells.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 375 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one injection or infusion of 375 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with two injections or infusions of 375 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with three or more injections or infusions of 375 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 100-750 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 200-750 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 300-700 mg/m 2 rituximab.
  • Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with 375 mg/m 2 rituximab.
  • This treatment can be repeated, once, twice or several times.
  • Rituximab can be injected or infused.
  • the pretreatment can be done 28-7 days before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to rituximab infused or injected once or twice 28-14 days before administration of 177 Lu-lilotomab satetraxetan.
  • An additional infusion or injection of rituximab can be done less than 4 hours before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to rituximab infused or injected once or twice 10-18 days before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to rituximab infused or injected once, twice, or three times at day 28, 21 or 14 before administration of 177 l_u-lilotomab satetraxetan.
  • Yet another embodiment of the present invention relates to 375 mg/m 2 rituximab infused or injected at 28 and 21 days before administration of 177 l_u-lilotomab satetraxetan.
  • a further embodiment of the present invention relates to 375 mg/m 2 rituximab infused or injected at 14 days before administration of 177 Lu-lilotomab satetraxetan.
  • Another embodiment of the present invention relates to 375 mg/m 2 rituximab infused or injected at 14 days and again less than 4 hours before administration of 177 Lu- lilotomab satetraxetan.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 40 mg/patient of lilotomab, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 40 mg/m 2 lilotomab, followed by 17.5 MBq/kg 177 Lu-lilotomab satetraxet
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 60 mg/m 2 lilotomab, followed by 20 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 25 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 30 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 35 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 45 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 50 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of INon-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 17,5 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 20 MBq/kg 177 l_u-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 25 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m 2 lilotomab, followed by 30 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days prior to administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days prior to administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab, followed by 17,5 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days prior to administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab, followed by 20 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days prior to administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab, followed by 25 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • An aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 1 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days prior to administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab, followed by 30 MBq/kg 177 l_u-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 17,5 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 20 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 25 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 30 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 l_u-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of lilotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 l_u-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of lilotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 17,5 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of lilotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 20 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of lilotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 25 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • a further aspect of the present invention relates to a combination of lilotomab and 177 Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 l_u-lilotomab satetraxetan, followed by 30 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Yet another aspect of the present invention relates to lilotomab for use in the reduction of haematological toxicity due to the administration of 177 l_u-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 100 mg/m 2 .
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 17,5 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 20 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 25 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m 2 rituximab 14 days before administration of 177 Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, predosing of 100 mg/m 2 lilotomab less than 4 hours before administration of 177 Lu-lilotomab satetraxetan, followed by 30 MBq/kg 177 Lu-lilotomab satetraxetan to a person in need thereof.
  • the therapy or treatment of the present invention can be administered either as a monotherapy or in combination with other therapies, preferentially standard treatments.
  • An aspect of the present invention relates to the treatment patterns shown in Arm 1 of figure 8.
  • An aspect of the present invention relates to the treatment patterns shown in Arm 2 of figure 8.
  • An aspect of the present invention relates to the treatment patterns shown in Arm 3 of figure 8.
  • An aspect of the present invention relates to the treatment patterns shown in Arm 4 of figure 8.
  • Pre-medication consisting of an antipyretic and antihistamine medication can be administered before infusion of rituximab.
  • the types of pre-medication are in accordance with each hospital's routine, including any use of corticosteroids.
  • Antibodies and radioimmunoconjugates are usually applied in the treatment of diseases formulated in pharmaceutical compositions.
  • compositions are optimized for parameters such as physiological tolerance and shelf-life.
  • the radioimmunoconjugates and/or antibodies of the present invention formulated as a pharmaceutical composition.
  • An embodiment of the present invention relates to a pharmaceutical composition as described above, further comprising one or more additional therapeutic agents.
  • a buffer solution which to a substantial degree maintain the chemical integrity of the radioimmunoconjugate and/or antibody and is being physiologically acceptable for infusion into patients.
  • the pharmaceutical composition comprises one or more pharmaceutically acceptable carriers and/or adjuvants.
  • Acceptable pharmaceutical carriers include but are not limited to non-toxic buffers, fillers, isotonic solutions, etc. More specifically, the pharmaceutical carrier can be but are not limited to normal saline (0.9 %), half-normal saline, Ringer's lactate, 5 % Dextrose, 3.3 % Dextrose/0.3 % Saline.
  • the physiologically acceptable carrier can contain a radiolytic stabilizer, e.g., ascorbic acid, which protect the integrity of the radiopharmaceutical during storage and shipment.
  • Betalutin formulated as indicated in Tables 1 and 2 in Example 1.
  • Preferably are sodium dihydrogen phosphate monohydrate, sodium chloride, recombinant human albumin, sodium ascorbate, diethylenetriamine pentaacetic acid (DTPA) and sodium hydroxide used as excipients in the formulation buffer.
  • DTPA diethylenetriamine pentaacetic acid
  • recombinant human albumin included in the formulation buffer as a stabilizer for the lilotomab satetraxetan conjugate.
  • the albumin also acts as a radioprotectant.
  • Recombinant human albumin structurally identical to human serum albumin derived from yeast is used. No human- or animal-derived raw material is involved in its manufacture. The excipient is well known and is used in pharmaceutical products for human use.
  • Betalutin is DTPA introduced as an excipient in the Betalutin formulation to chelate any free 177 Lu 3+ ions and to reroute this impurity from accumulation in the bone to rapid renal clearance (Li et al 2001, Breeman et al 2003).
  • Betalutin contains 9.3 ⁇ DTPA in 12 mL, while the maximum amount of no-carrier added (n.c.a) 177 Lu 3+ (> 3,000 GBq/mg) applied (6.9 GBq) corresponds to less than 15 nmol Lu ions. This gives a more than 1000-fold molar excess of DTPA over Lu 3+ ions.
  • the formulation buffer an aqueous solution with pH 6.9 to 7.0 and thus no incompatibilities between the drug substance and the formulation buffer are expected.
  • One embodiment of the present invention comprises the pharmaceutical composition of the present invention and one or more additional antibodies or radioimmunoconjugates.
  • a pharmaceutical composition comprising (per mL) : 0.75 mg Lutetium ( 177 Lu) lilotomab satetraxetan, 0.46 mg Ammonium acetate, and Trace amounts of HCb.
  • Another aspect of the present invention relates to a pharmaceutical composition
  • a pharmaceutical composition comprising (per mL): 30.86 mg Sodium ascorbate, 0.31 mg DTPA, 0.17 mg NaOH, 60.82 mg Recombinant human albumin, 3.32 mg Sodium dihydrogen phosphate monohydrate, and 4.34 mg Sodium chloride with the pH is adjusted to 6.9-7.0.
  • a further aspect of the present invention relates to a pharmaceutical composition
  • a pharmaceutical composition comprising;
  • the present invention also relates to the pharmaceutical compositions of the present examples, as well as the dosage administration patterns presented herein. This includes the use of the pharmaceutical compositions of the present invention for use in the treatment of Non-Hodgkin lymphoma.
  • the person in need of treatment with 177 Lu-lilotomab satetraxetan is suffering from a CD37 related disease, typically a B-cell lymphoma such as Non-Hodgkin lymphoma (NHL).
  • a CD37 related disease typically a B-cell lymphoma such as Non-Hodgkin lymphoma (NHL).
  • NHL Non-Hodgkin lymphoma
  • NHL is a group of blood cancers that includes all types of lymphoma except Hodgkin's lymphomas. Symptoms include enlarged lymph nodes, fever, night sweats, weight loss, and feeling tired. Other symptoms may include bone pain, chest pain, or itchiness. Some forms are slow growing while others are fast growing.
  • lymphoma being a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, Diffuse large B-cell lymphoma, and mantle cell.
  • the NHL cancer follicular grade I-IIIA In an embodiment of the present invention is the NHL cancer marginal zone.
  • the present invention is the NHL cancer small lymphocytic.
  • the NHL cancer lymphoplasmacytic In an embodiment of the present invention is the NHL cancer mantle cell.
  • the present invention is the NHL cancer AML.
  • the NHL cancer CLL In an embodiment of the present invention is the NHL cancer CLL. In an embodiment of the present invention is the NHL cancer Diffuse Large B-cell lymphoma (DLBCL).
  • LLBCL Large B-cell lymphoma
  • leukemia also express the CD37 antigen.
  • another embodiment of the present invention relates to leukemia of the subtypes chronic lymphocytic leukemia and acute myelogen leukemia. More specifically the present invention relates to AML with 11Q23/MLL translocation.
  • the present invention is the NHL cancer AML with 11Q23/MLL translocation.
  • Betalutin is an antibody-radionuclide-conjugate (ARC) composed of the radioisotope lutetium-177, the linker benzyl-DOTA and the murine anti-CD37 IgGl antibody, lilotomab.
  • the active moiety is the beta particle emitting nuclide 177 Lu.
  • Lutetium-177 has physical half-life of 6.7 days.
  • the antibody lilotomab recognises epitopes on the CD37 antigen, which is abundant on the cell surface of tumours of B-cell origin, including NHL.
  • Betalutin is prepared as a solution for intravenous administration. 1 mg/ml lilotomab antibody will be used, between 7 to 20 mg lilotomab antibody per patient.
  • the amount of lutetium ( 177 Lu)-lilotomab satetraxetan injected per patient will depend on dose level and patient's weight; however, the dose is capped for patients who weigh more than 130 kg (patients heavier than 130 kg will receive the dose for a 130 kg patient).
  • Betalutin are supplied in vials containing a ready to use solution.
  • the investigational medicinal product will be referred to as Betalutin or lutetium ( 177 Lu)- lilotomab satetraxetan in the protocol.
  • Rituximab (MabThera) is used as pre-treatment.
  • Rituximab a chimeric anti-CD20 antibody will be used to clear the circulating normal peripheral B-lymphocytes in the blood and in the spleen before administrating CD37 targeting Betalutin. This may secure better access for Betalutin to less accessible compartments such as lymph nodes and larger tumour masses.
  • Rituximab targets CD20 and will not block the binding of Betalutin CD37 on the B-lymphocytes or tumour cells.
  • Betalutin contains a murine monoclonal antibody which has been shown from in vitro analysis to bind to the human Fc-y receptor Ila.
  • rituximab binds to CD20 it also binds to the Fc-y receptor Ila and if administered just prior to Betalutin may therefore inhibit the binding of Betalutin to this receptor and improve its biodistribution.
  • Arm 3 has therefore been included in the study via a protocol amendment to test the ability of rituximab to improve the biodistribution of Betalutin. This improved biodistribution may reduce the incidence of myleosuppressive adverse events by decreasing the radioactivity in the bone marrow and spleen.
  • Phase I arms 1, 2, and Phase II two intravenous infusions of 375 mg/m 2 rituximab have been given, at 28 Days and 21 Days, before administration of Betalutin.
  • arms 3, 4 and 5 one intravenous infusion of 375 mg/m2 rituximab have been given 14 days before, and in arms 3 and 5 an additional intravenous infusion of 375 mg/m 2 rituximab will be given within 4 hours before Betalutin administration on Day 0.
  • Premedication consisting of an antipyretic and antihistamine medication should be administered before infusion of rituximab.
  • the types of pre-medication are in accordance with each hospital's routine, including any use of corticosteroids.
  • Lilotomab is used as pre-dosing.
  • One intravenous infusion of 40 mg lilotomab in arm 1, and 100 mg/m 2 lilotomab in arm 4 and arm 5, is performed within 4 hours before administration of Betalutin (up to a maximum of 2.7m 2 for lilotomab in arm 4 and 5).
  • Pre-medication consisting of an antipyretic and antihistamine medication should be administered before infusion of lilotomab.
  • Betalutin is administered in a dose of 15-20 Mbq/kg. Arm 4 is 15 Mbq/kg.
  • Platelet and neutrophil counts of arm 3 (rituximab predosing) and arm 4 (100 mg/m 2 lilotomab predosing) show grade 3-4 toxicity of arm 3 and no toxicity of arm 4 (figures 1 and 2).
  • the PK profiles show a large separation between the treatment arms.
  • Arm 1 40 mg lilotomab predosing
  • Arm 2 no predosing
  • Arm 3 rituximab predosing
  • Arm 4 100 mg/m 2 lilotomab predosing (figure 3).
  • Phase I arms 3 and 4
  • one intravenous infusion of 375 mg/m2 rituximab have been given 14 days before, and in arm 3 an additional intravenous infusion of 375 mg/m2 rituximab have been given within 4 hours before Betalutin administration on
  • Pre-medication consisting of an antipyretic and antihistamine medication should be administered before infusion of rituximab.
  • the types of premedication are in accordance with each hospital's routine, including any use of corticosteroids.
  • Lilotomab is used as pre-dosing.
  • the same antibody, lilotomab, as used in Betalutin, a murine anti-CD37 antibody, is used to block the binding on remaining B-cells, after rituximab treatment, in the lymphoid organs.
  • Pre-medication consisting of an antipyretic and antihistamine medication should be administered before infusion of lilotomab.
  • Betalutin is administered in a dose of 15-20 MBq/kg.
  • Platelet and neutrophil counts of patients in arm 1 show grade 3-4 toxicity of arm 2 and 3, less toxicity of arm 1 and no toxicity of arm 4 (figures 5 and 6).
  • the PK profiles show a large separation between the treatment arms.
  • Arm 1 40 mg lilotomab predosing
  • Arm 2 no predosing
  • Arm 3 rituximab predosing
  • Arm 4 100 mg/m2 lilotomab predosing (figure 7).
  • Aim Four different combinations of pre-dosing and pre-treatment have been investigated. All patients were pre-treated with different regimens of rituximab. Two arms included cold lilotomab pre-dosing (arm 1 and 4; 40 mg fixed and 100 mg/m 2 Body Surface Area dosage, respectively) and two did not (arm 2 and 3). Patients received either 10, 15 or 20 MBq 177 Lu-lilotomab satetraxetan per kg body weight. Previously, we have shown that absorbed red marrow (RM) doses were lower in arml vs arm2, and that haematological toxicity was more severe for patients receiving higher RM doses. The aim of this work was to compare the ratios of tumour to RM absorbed doses between arm 1, 4 and non-pre-dosed patients (arm 2 + 3).
  • RM red marrow
  • RM dosimetry A total of 16 patients were included for RM dosimetry, of these were 14 included for tumour dosimetry. A total of 35 tumours were included, 1 to 5 from each patient (mode 3). RM and mean tumour absorbed doses per administered activity were determined from multiple SPECT/CT-images for each patient. Two-sided student-t- tests were used for all statistical analyses. Results:
  • Mean tumour absorbed doses were 1.62, 2.78 and 1.37 mGy/MBq for arm 1, 4 and non-pre-dosing
  • Pre-dosing with lilotomab has a mitigating effect on red marrow absorbed dose for 177 Lu- lilotomab satetraxetan patients, and increased amounts was found correlated with a higher tumour dose. Both pre-dosage levels significantly increased the tumour to RM absorbed dose ratio.
  • the key eligibility criteria was: 1) Age >18 with histologically confirmed relapsed indolent B-cell NHL (follicular grade I-IIIA, mantle cell, SLL, marginal zone,
  • lymphoplasmacytic subtypes 2) ⁇ 25% bone marrow involvement. 3) Life expectancy >3 months. 4) Platelet count > 150 x 10 9 /L. 5) ANC >1.5 x 10 9 /L. 6) No previous hematopoietic stem cell transplantation. Dose-limiting toxicities (DLTs) were assessed during the first 12 weeks. Incidence and severity of adverse events (AEs) according to common terminology criteria for adverse events (CTCAE) v4.0. Response assessments were conducted at 3, 6 (FDG PET-CT), 9, 12, 18, 24 and 36 months (CT) per the International Working Group (IWG) criteria for NHL.
  • IWG International Working Group
  • the hematological toxicity was reduced by pre-dosing with lilotomab.
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20-250 mg/m 2 lilotomab, followed by
  • 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-2, wherein 177 Lu-lilotomab satetraxetan is administered at a concentration 15 MBq/kg. 4. 177 l_u-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-3, wherein 177 Lu-lilotomab satetraxetan is administered at a concentration 17,5 MBq/kg.
  • 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-4, wherein 177 Lu-lilotomab satetraxetan is administered at a concentration 20 MBq/kg.
  • Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-5, wherein lilotomab is administered at a concentration selected from the group consisting of 20 mg/m 2 , 40 mg/m 2 , 50 mg/m 2 , 60 mg/m 2 , 75 mg/m 2 , 100 mg/m 2 , 125 mg/m 2 , 150 mg/m 2 , 200 mg/m 2 , 250 mg/m 2 , 20 mg/patient and 40 mg/patient.
  • Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-8, wherein lilotomab is administered at 60 mg/m 2 .
  • Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-9, wherein lilotomab is administered at 40 mg/patient.
  • 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to item 14, wherein 375 mg/m 2 rituximab is administered at 28 and 21 days before administration of 177 Lu-lilotomab satetraxetan.
  • 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to item 14, wherein 375 mg/m 2 rituximab is administered at 14 days before administration of 177 Lu-lilotomab satetraxetan.
  • 177 Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to items 14 and 16, wherein 375 mg/m 2 rituximab is infused at 14 days before and again less than 4 hours before administration of 177 Lu-lilotomab satetraxetan. 18.
  • Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-17, wherein the lymphoma is a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, AML, CLL, BLBCL, AML with 11Q23/MLL translocation, and mantle cell.
  • Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-12, wherein the patient is relapsing after treatment with rituximab.
  • Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20-250 mg/m 2 lilotomab, followed by
  • Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to item 20-21, wherein 177 Lu-lilotomab satetraxetan is administered at a concentration 10 MBq/kg.
  • Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein 177 Lu-lilotomab satetraxetan is 3administered at a concentration 20 MBq/kg.
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 20-250 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 40 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 100 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 177 Lu-lilotomab satetraxetan according to items 57-61, wherein ⁇ Lu- lilotomab satetraxetan is administered in a dose of 17,5 MBq/kg.
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 100 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 100 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 100 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 60 mg/m 2 .
  • Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177 Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177 Lu-lilotomab satetraxetan in a dose of 60 mg/m 2 .
  • Non-Hodgkin lymphoma comprising administration of 177 Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 20-250 mg/m 2 lilotomab, followed by
  • Non-Hodgkin lymphoma comprising administration of 177 Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 20-500 mg/m 2 lilotomab, followed by
  • a method of treating Non-Hodgkin lymphoma comprising administration of 177 Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 40 mg/m 2 lilotomab, followed by
  • a method of treating Non-Hodgkin lymphoma comprising administration of 177 Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 40 mg/patient lilotomab, followed by
  • a method of treating Non-Hodgkin lymphoma comprising administration of 177 Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 100 mg/m 2 lilotomab, followed by
  • a method of treating Non-Hodgkin lymphoma comprising administration of 177 Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 100 mg/m 2 lilotomab, followed by
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m 2 rituximab administered at 14 days before administration of 177 Lu-lilotomab satetraxetan,
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m 2 rituximab administered at 14 days before administration of 177 Lu-lilotomab satetraxetan,
  • 177 Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177 Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :

Abstract

The disclosure relates to the use of 177Lu-lilotomab satetraxetan in the treatment of Non-Hodgkin lymphoma. Aspects included are specific administration patterns, with specific concentrations, pre-treatments and predosing.

Description

Treatment of Non-Hodgkin Lymphoma using lilotomab and 177Lu-lilotomab satetraxetan
FIELD OF THE INVENTION
The invention relates to the use of monoclonal antibodies conjugated with 177Lu in the treatment of Non-Hodgkin lymphoma. Aspects included specific administration patterns, with specific concentrations, pre-treatments and predosing, wherein 177Lu- lilotomab satetraxetan is the central medicament.
BACKGROUND OF THE INVENTION
Non-Hodgkin Lymphomas (NHL) as a group is the most common malignant
haematological disease. NHLs are a diverse group of blood cancers that include any kind of lymphoma except Hodgkin lymphoma. NHLs are tumours developed from lymphocytes, a type of white blood cells. NHLs vary in their clinical behaviour, morphologic appearance, immunologic and molecular phenotype. The various types represent neoplastic lymphoid cells arrested at different stages of differentiation.
Based on their natural history, NHLs can be clinically classified as indolent, aggressive, and highly aggressive. Diffuse large B-cell and follicular lymphoma are the most common subtypes.
NHLs are the fifth most common cause of cancer in the United States, with an estimated incidence of 70,130 cases in 2012. Follicular center cell lymphomas are the second most common subtype, comprising approximately 40% of all NHLs. Since 1950, the incidence of NHL has steadily increased at approximately 4% per year. Treatment usually depends on the type of lymphoma and its stage, as well as other prognostic factors. The different treatment options are radiation therapy,
chemotherapy, immunotherapy, radioimmunotherapy (RIT) and bone marrow or peripheral stem cell transplantation. In B-cell and follicular lymphoma, rituximab (immunotherapy) combined with chemotherapy or a combination of drugs such as CHOP (cyclophosphamide, hydroxydaunorubicin, Oncovin and prednisone) regimen is used.
Patients with relapsed indolent lymphoma may repeatedly respond to rituximab, chemotherapy combined with rituximab or other chemotherapy combinations although the proportion responding decreases with each relapse. The aim of RIT is to use a monoclonal antibody (MoAb) to target an isotope for radiation to tumour tissue while limiting the toxicity to normal cells. Beta-emitting radioimmunoconjugates (RIC) possess high levels of clinical activity in patients with relapsed or refractory B-cell lymphomas, including those refractory to rituximab and chemotherapy. Clinical data have validated that RIT is both more cost effective and more efficacious than nonradioactive immunotherapy. More recently, several single- arm studies have demonstrated that upfront RIT administered either alone or with chemotherapy to previously untreated indolent NHL patients produces overall response rates of 90-100 %, complete response rates of 60-95 % and durable remissions.
A phase III study of RIT as part of frontline therapy for indolent NHL reported that consolidation therapy with 90Y-ibritumomab tiuxetan (Zevalin) after induction chemotherapy markedly prolonged progression free survival in patients with previously untreated stage II or IV follicular lymphoma. In another study, patients with indolent and aggressive NHLs received four cycles of chemotherapy followed by high myeloablative dose 90Y-ibritumomab tiuxetan followed by autologous stem cell support. After a follow up time of 30 months, the overall survival rate was 87 % and the event free survival was 69 %. Although myeloablative doses of 90Y-ibritumomab tiuxetan were given, the RIT was well tolerated. The low dose-rate permits RIT to be effective for haematologic malignancies while causing minimal non-haematological toxicity. When anti-CD20 RIT is given to patients, they are administered with large quantities of unlabeled cold anti-CD20 antibody immediately before radiolabelled anti-CD20 antibodies. Such a priming dose is necessary to optimize radiolabelled antibody concentrations in tumour, presumably by partially saturating easily accessible B-cells in the blood and the spleen and permitting sufficient radiolabelled antibody to bypass these sites and penetrate less accessible compartments such as lymph nodes and large tumour masses.
However, too much cold anti-CD20 antibody over a long time can result in blocking of the CD20 antigen on tumour cells and thus reduce the effect of anti-CD20 RIT. Both clinical and non-clinical studies have shown that in some circumstances quite low rituximab concentrations in the blood can reduce tumour cell targeting and thus impair the clinical efficacy of CD20-directed RIT. A solution to this problem might be to omit cold rituximab from the last cycles of therapy before RIT. Alternatively; one could choose to target another B-cell surface antigen such as CD37.
RIT with CD37 as the target antigen has been explored previously using a 131I-labeled murine monoclonal antibody (MB-1) both in a mouse model and in patients with low, intermediate and high-risk NHLs. CD37 antibodies were compared with CD20 antibodies and a higher grade of internalization and degradation of 131I-labeled RIC was found for CD37 than for CD20. Furthermore, a favorable biodistribution was obtained in 59 % of the patients for CD20 and for 50 % of the patients for CD37. The amount of cold priming with antibody necessary to get a favorable biodistribution was higher for CD37 than for CD20. All six patients treated with 131I-MB-1 (against CD37 antibody) had a complete response and three of the patients received bone marrow transplantation. Of twelve patients that were treated with 131I labeled antibody against CD20 ten had a complete response and eleven needed bone marrow transplantation. Despite the clinical responses observed in this study, the data for CD20 was evaluated to be marginally better than for CD37. CD20 was therefore chosen as the target antigen for further development of a commercially available radioimmunoconjugate (RIC). This development resulted in FDA approval of Bexxar and Zevalin in 2003. No subsequent efforts have been made to target CD37 with RICs. Trubion Pharmaceuticals have however developed a nonradioactive CD37-binding small modular immunopharmaceutical that induces apoptosis and antibody-dependent cellular cytotoxicity against B-cell
leukemia/lymphoma cell lines and primary chronic lymphocytic leukaemia cells.
Previous studies thus show that CD37 is a potent target for both immunotherapy and RIT. The chloramine T method of 131I-labeling was used in the early studies of CD37 RIT described above. 131I labeled to antibodies with the iodogen or the chloramine T method are not being contained in the cells if the antigen-antibody complex is internalized. Inside the cells the nuclide is removed from the antibody by intracellular enzymes and diffuses out and away from the tumour cells. The same so-called dehalogenation has been shown with CD22 antibodies, which are also internalized. Metallic radionuclides labeled to antibodies with so-called chelators are however more stable and remain contained inside the cells to a much higher degree. By using metallic radionuclides internalizing antigens can be used for tumour targeting and tumour uptake may also be higher than for non-internalizing antibodies as well.
At the Norwegian Radium Hospital, an antibody (lilotomab also called HH1) was developed against CD37 in the 1980's. Lilotomab and the anti-CD20 antibody rituximab have been labeled with both 125I and mIn and measured cell bound activity after 4 days of incubation with a lymphoma cell line. The results show that the problem of catabolism of RIC can be circumvented by labeling with metallic nuclides such as mIn or 177Lu.
The most common radiopharmaceuticals used in therapy today utilize substances that disintegrate resulting in the emission of a beta particle. Beta particles are electrons emitted from the nucleus of an atom. Beta emitters approved for therapy include
Iodine-131 (TVi = 8 days), Yttrium-90 (TVi = 2.7 days) and Lutetium-177 (JVi = 6.7 days). 177Lu has been selected for use in Betalutin since it has proven to be suitable for labeling of the antibody and has an appropriate energy of the emitted β-particle (Emax = 0.497 MeV, T1/2 = 6.7 days). Furthermore, it has a low abundance of photons with almost ideal energy for imaging (E = 113 keV, abundance = 6.5 %; E = 208 keV, abundance = 11 %).
Betalutin (lilotomab labeled with 177Lu via the chelator p-SCN-benzyl-DOTA, or 177Lu- lilotomab satetraxetan) has been developed by Nordic Nanovector in collaboration with the Norwegian Radium Hospital for the treatment of relapsed NHL.
RIT permits delivery of a therapeutic dose of radiation directly to the DNA of tumour cells. The radionuclide 177Lu is a beta-particle emitter. The beta particles are electrons with energy and range in tissue suitable for treating NHLs. The absorbed radiation results in DNA damage and tumour cell death. The radiation emitted from the radiolabeled antibody affects not only the antibody-binding cell, but also neighbouring cells. This mechanism of action of RIT may be especially beneficial in treating patients with bulky or poorly vascularized tumours. Betalutin has been tested for targeting, therapeutic and toxic effect in cells and in mice. Lilotomab has similar or better binding properties to CD37 as rituximab has to CD20. Therapy against single cells showed a significantly better effect of Betalutin than of 177Lu-rituximab. The MTD of Betalutin in SCID mice with tumour cells in the bone marrow was between 50 and 100 MBq/kg (Dahle et al. 2013). In studies with nude mice without tumour cells in the bone marrow the MTD is above 500 MBq/kg (Repetto et al. 2015).
Biodistribution studies with Betalutin have shown high uptake in tumour and uptake in normal organs similar to the uptake of 177Lu-rituximab. The preclinical data to date indicate that Betalutin has a suitable biodistribution profile with high uptake in tumour cells, and that the efficacy results in the mouse models show promise of potentially interesting clinical results.
Thus, 177Lu-lilotomab satetraxetan is a candidate for the treatment of Non-Hodgkin lymphoma. However, there are serious challenges before 177Lu-lilotomab satetraxetan can be used in the general population.
These are related to issues related to for example haematological toxicity of 177Lu- lilotomab satetraxetan, and to finding the optimal way of having higher activity levels of 177Lu-lilotomab satetraxetan in order to obtain a higher probability of obtaining partial or complete responses in the patients.
These challenges have now surprisingly been overcome.
SUMMARY OF THE INVENTION
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m2 lilotomab, followed by 10-50 MBq/kg 177l_u-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising predosing of 20-250 mg/m2 lilotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. A further aspect of the present invention relates to a combination of lilotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m2 lilotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Yet another aspect of the present invention relates to lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 20- 250 mg/m2.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of 177Lu-lilotomab satetraxetan in an administration pattern comprising predosing of 20-250 mg/m2 lilotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An embodiment of the present invention relates to 177l_u-lilotomab satetraxetan administered at a concentration selected from the group consisting of 10, 12,5, 15, 17.5, 20, 25, 30, 35, 40, 45 and 50 MBq/kg.
Another embodiment of the present invention relates to lilotomab administered at a concentration selected from the group consisting of 20, 40, 50, 60, 75, 100, 125, 150, 200, 250 mg/m2. A further embodiment of the present invention relates to the predosing of lilotomab done less than 24 hours, such as within 4 hours, before administration of 177Lu-lilotomab satetraxetan.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more infusions of 375 mg/m2 rituximab.
Yet another embodiment of the present invention relates to 375 mg/m2 rituximab infused at 28 and 21 days before administration of 177Lu-lilotomab satetraxetan. A further embodiment of the present invention relates to 375 mg/m2 rituximab infused at 14 days before administration of 177Lu-lilotomab satetraxetan.
Another embodiment of the present invention relates to 375 mg/m2 rituximab infused at 14 days and within 4 hours before administration of 177Lu-lilotomab satetraxetan.
Another embodiment of the present invention relates to the lymphoma being a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, and mantle cell. BRIEF DESCRIPTION OF THE FIGURES
Figure 1 shows platelet counts of arm 3 (rituximab predosing) and arm 4 ( 100 mg/m2 lilotomab predosing). The patients in arm 3 suffers grade 3-4 hematological toxicity while there is no toxicity in arm 4.
Figure 2 shows neutrophil counts of arm 1 (40 mg lilotomab predosing), arm 3 (rituximab predosing) and arm 4 ( 100 mg/m2 lilotomab predosing). The patients in arm 3 suffers grade 3-4 toxicity, while there is no toxicity of arm 4 and arm 1 is in between.
Figure 3 shows PK profiles that show a large separation between the treatment arms. Arm 1 = 40 mg lilotomab predosing, Arm 2 = no predosing, Arm 3 = rituximab predosing and Arm 4 = 100 mg/m2 lilotomab predosing.
Figure 4 shows an example of an administration pattern.
Figure 5 shows platelet counts of patients in arm 1 (40 mg predosing), arm 2 (no predosing), arm 3 (rituximab predosing) and arm 4 (100 mg/m2 lilotomab predosing). There was grade 3-4 toxicity of arm 2 and 3, less toxicity of arm 1 and no toxicity of arm 4.
Figure 6 shows neutrophil counts of patients in arm 1 (40 mg predosing), arm 2 (no predosing), arm 3 (rituximab predosing) and arm 4 (100 mg/m2 lilotomab predosing). There was grade 3-4 toxicity of arm 2 and 3, less toxicity of arm 1 and no toxicity of arm 4.
Figure 7 shows PK profiles that show a large separation between the treatment arms. Arm 1 = 40 mg lilotomab predosing, Arm 2 = no predosing, Arm 3 = rituximab predosing and Arm 4 = 100 mg/m2 lilotomab predosing.
Figure 8 shows examples of an administration patterns tested. Figure 9 shows that the mean values for platelets and neutrophils at nadir for 23 arm 1 patients were lower than the mean values for 3 arm 4 patients.
Figure 10 shows dose limiting toxicity and number of grade 3 and 4 adverse events were lower for arm 4 than for arm 1 and highest for arm 2.
Figure 11 shows the response rates for each to the tested administration patterns.
Figure 12 shows four different combinations of pre-dosing and pre-treatment that have been investigated. Two arms included cold lilotomab pre-dosing (arm 1 and 4; 40 mg fixed and 100 mg/m2 Body Surface Area dosage, respectively) and two did not (arm 2 and 3). Pre-dosing with lilotomab has a mitigating effect on red marrow absorbed dose for 177Lu-lilotomab satetraxetan patients, and increased amounts was found correlated with a higher tumour dose.
Figure 13 shows mean platelet count in Arms 1 and 4 for 15 and 20 MBq/kg 177Lu- lilotomab satetraxetan.
Figure 14 shows mean neutrophil count in Arms 1 and 4 for 15 and 20 MBq/kg 177Lu- lilotomab satetraxetan.
DETAILED DESCRIPTION OF THE INVENTION
The present invention relates to the treatment of Non-Hodgkin lymphoma using 177Lu- lilotomab satetraxetan with lilotomab and with or without rituximab, where the inventors surprisingly have found that a specific treatment pattern have advantageous effects.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma or other CD37 positive blood cancers, wherein 177Lu-lilotomab satetraxetan is administered according to a clinically relevant administration pattern comprising 10-20 MBq/kg 177Lu-lilotomab satetraxetan, to a person in need thereof.
The clinically relevant administration pattern can be seen as an administration pattern that has clinical relevance and effect on human individuals suffering from Non-Hodgkin lymphoma.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177l_u-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20- 100 mg/m2 lilotomab, followed by b) 10-20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. In the present context can the term treatment be seen as the partial of full treatment of cancer, including any amelioration and for example stabilization of progressing disease.
Thus, the term treatment may be seen as an improvement of any of the criteria tested in the examples of the present disclosure. One criteria is overall response rate (ORR). Another is complete response (CR). A further is partial response (PR). Another is stable disease (SD).
The lilotomab predosing effect is likely caused by blocking of the binding on remaining B-cells in the lymphoid organs. This can be more effective after rituximab treatment.
Pre-medication consisting of an antipyretic and antihistamine medication can be administered before infusion of lilotomab. Thus, an aspect of the present invention relates to 177Lu-lilotomab satetraxetan and lilotomab for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to a specific administration pattern.
Method of treatment and for use in treatment
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m2 lilotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
The predosing of 20-250 mg/m2 lilotomab may be substituted with 40-500 mg/patient in all aspects and embodiments of the invention.
A further aspect of the present invention relates to lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising predosing of 20-250 mg/m2 lilotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. A further aspect of the present invention relates to a combination of Iiiotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein Iiiotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 20-250 mg/m2 Iiiotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Yet another aspect of the present invention relates to Iiiotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan, wherein Iiiotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 20- 250 mg/m2.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of 177Lu-lilotomab satetraxetan in an administration pattern comprising predosing of 20-250 mg/m2 Iiiotomab, followed by 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
The therapy or treatment of the present invention can be administered either as a monotherapy or in combination with other therapies, preferentially standard treatments.
Such other therapies may be one or more selected from the group consisting of pretreatment, surgery, chemotherapy (including doxorubicin, vinblastin and gemcitabine), immunotherapy, antibody therapy, photodynamic therapy, proteasome inhibitor (including bortezomib), histone deacetylase inhibitors (including vorinostat and suberoylanilide hydroxamic acid), vitamin D3 and vitamin D3 analogs, cell cycle checkpoint inhibitors (including UCN-01 and 2-(4-(4-Chlorophenoxy)phenyl)-lH- benzimidazole-5-carboxamide), hypoxic cell radiosensitizers (including metronidazole and misonidazole), apoptosis inducers (including withaferin A and venetoclax), radiosensitizers, radioimmunotherapy or a combination of two or more of these.
In one embodiment of the present invention has the patient being treated according to the present invention already been undergoing treatment for cancer.
In one embodiment of the present invention is this treatment of therapy one or more of those mentioned above. In a preferred embodiment is the therapy rituximab, and in this case can the patient be a patient relapsing after rituximab treatment.
Thus, an embodiment of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to the present invention, wherein the patient is relapsing after treatment with rituximab. Lilotomab and 177Lu-lilotomab satetraxetan
The monoclonal antibody (mAb or moAb) lilotomab was previously known as tetulomab or HH 1 while 177Lu-lilotomab satetraxetan was previously known as 177Lu-labeled HH 1 antibody, or named 177Lu-tetulomab or by the tradename Betalutin.
177Lu-lilotomab satetraxetan is a radioimmunoconjugate (RIC) also known as antibody radionuclide conjugate (ARC) that is capable of binding to or targeting an antigen of interest. In the present case is this antigen CD37.
Satetraxetan is a derivative of DOTA, p-SCN-benzyl-DOTA.
Administration route
By administered is meant intravenous infusion or intravenous injection. More specifically, the radioimmunoconjugate and antibody of the present invention can be administered directly in a vein by a peripheral cannula connected to a drip chamber that prevents air embolism and allows an estimate of flow rate into the patient.
In one embodiment the radioimmunoconjugate and/or antibody can be administered in a repeated fashion.
In another embodiment the radioimmunoconjugate followed by monoclonal antibody (or immunoconjugate) can both be administered in a repeated fashion.
An embodiment of the present invention relates to the use of the radioimmunoconjugate and/or antibody of the present invention administered in combination with or in addition to other therapy.
In an embodiment of the present invention the other therapies are selected from pretreatment, chemotherapy, monoclonal antibody therapy, surgery, radiotherapy, and/or photodynamic therapy.
In another embodiment of the present invention the other therapies are bone marrow transplantation or stem cell transplantation and/or therapy.
Administration dosages
In the present invention is 177Lu-lilotomab satetraxetan used in the treatment of Non- Hodgkin's lymphoma. An embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration selected from the group consisting of 10, 12,5, 15, 17.5, 20, 25, 30, 35, 40, 45, 50 MBq/kg. An embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 10 MBq/kg.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 12,5 MBq/kg.
A further embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 17,5-20 MBq/kg.
Yet another embodiment of the present invention relates to 177l_u-lilotomab satetraxetan administered at a concentration of 20-25 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 25-30 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 30-35 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 35-40 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 40-45 MBq/kg.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 45-50 MBq/kg.
Lilotomab is used for predosing before administration of 177Lu-lilotomab satetraxetan. An embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 2-50 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 100 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 120 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 150 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 200 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 20 mg/m2.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/m2.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 60 mg/m2.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 20 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 20 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 20 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg. Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/m2 followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/patient followed by 177l_u-lilotomab satetraxetan administered at a concentration of 15 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 40 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 100 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 50 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
Another embodiment of the present invention relates to predosing of lilotomab administered at a concentration of 60 mg/patient followed by 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg.
A further embodiment of the present invention relates to lilotomab administered at a concentration of 50 mg/m2. This may in an embodiment of the invention be equal to 100 mg/patient.
A further embodiment of the present invention relates to lilotomab administered at a concentration of 60 mg/m2. This may in an embodiment of the invention be equal to 120 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 75 mg/m2. This may in an embodiment of the invention be equal to 150 mg/patient. Yet another embodiment of the present invention relates to lilotomab administered at a concentration of 100 mg/m2. This may in an embodiment of the invention be equal to 200 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 125 mg/m2. This may in an embodiment of the invention be equal to 250 mg/patient.
A further embodiment of the present invention relates to lilotomab administered at a concentration of 150 mg/m2. This may in an embodiment of the invention be equal to 300 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 175 mg/m2. This may in an embodiment of the invention be equal to 350 mg/patient.
A further embodiment of the present invention relates to lilotomab administered at a concentration of 200 mg/m2. This may in an embodiment of the invention be equal to 400 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 225 mg/m2. This may in an embodiment of the invention be equal to 450 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 40 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 50 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 60 mg/patient.
Yet another embodiment of the present invention relates to lilotomab administered at a concentration of 250 mg/m2. This may in an embodiment of the invention be equal to 500 mg/patient. Another embodiment of the present invention relates to lilotomab administered at a concentration of 20-250 mg/m2. This may in an embodiment of the invention be equal to 10-125 mg/patient. A further embodiment of the present invention relates to lilotomab administered at a concentration of 20-100 mg/m2. This may in an embodiment of the invention be equal to 40-200 mg/patient.
Another embodiment of the present invention relates to lilotomab administered at a concentration of 20-150 mg/m2. This may in an embodiment of the invention be equal to 40-300 mg/patient.
A further embodiment of the present invention relates to lilotomab administered at a concentration of 100-200 mg/m2. This may in an embodiment of the invention be equal to 200-400 mg/patient. Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 15-20 MBq/kg and lilotomab administered at a concentration of 20-100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 15-20 MBq/kg and lilotomab administered at a concentration of 40-100 mg/m2. This may in an embodiment of the invention be equal to 80-200 mg/patient.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 17,5-20 MBq/kg and lilotomab administered at a concentration of 40-100 mg/m2.
A further embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 30 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 35 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 40 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 45 MBq/kg and lilotomab administered at a concentration of 100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 50 MBq/kg and lilotomab administered at a concentration of 100 mg/m2. Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 30 MBq/kg and Iiiotomab administered at a concentration of 60 mg/m2.
A further embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 15 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 17,5 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 20 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
A further embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 25 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 30 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 35 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
A further embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 40 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2.
Another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 45 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2. Yet another embodiment of the present invention relates to 177Lu-lilotomab satetraxetan administered at a concentration of 50 MBq/kg and Iiiotomab administered at a concentration of 40-100 mg/m2. The PK profiles (e.g. figure 3) show activity in kBq/ml in the hours after 177Lu-lilotomab satetraxetan administration. A high concentration means that a high amount of 177Lu- lilotomab satetraxetan is present in the blood.
Thus, in one embodiment of the present invention is the activity (in kBq/ml) after 72 hours more than 80 kBq/ml, such as more than 70 kBq/ml, such as more than 60 kBq/ml.
In another embodiment of the present invention is the activity (in kBq/ml) after 48 hours more than 110 kBq/ml, such as more than 100 kBq/ml, such as more than 90 kBq/ml, such as more than 80 kBq/ml.
Haematological toxicity
The administration of immunosuppressive agents may be associated with the occurrence of hematologic toxicity, such as anemia, due to bone marrow suppression or hemolysis, leukopenia, neutropenia and thrombocytopenia.
Neutropenia is graded; grade 1 is Neutrophils <LLN to 1500/mm3, grade 2 is Neutrophils < 1500/mm3 to 1000/mm3, grade 3 is Neutrophils < 1000/mm3 to 500/mm3, and grade 4 is Neutrophils <500/mm3 (see also figure 2) Thrombocytopenia is graded; grade 1 is Platelets <LLN to 75,000/mm3, grade 2 is <75,000/mm3 to 50,000/mm3, grade 3 is <50,000/mm3 to 25,000/mm3, and grade 4 is <25,000/mm3 (see also figure 1).
Preferably is no neutropenia grade 4 observed after the treatment, and even more preferably is no grade 3 or 4 observed 45 days after the treatment.
Preferably is no thrombocytopenia grade 4 observed after the treatment, and even more preferably is no grade 3 or 4 observed 45 days after the treatment.
In one embodiment is no grade 3 or 4 neutropenia and thrombocytopenia or no grade 3 neutropenia and thrombocytopenia observed 45 days after the treatment. Neutropenia and thrombocytopenia in patients can for example be seen in example 1 and figures 1 and 2.
An aspect of the present invention relates to the use of lilotomab to reduce hematologic toxicity such as neutropenia and/or thrombocytopenia in patients suffering from non- Hodgkin's lymphoma. These patients may previously be treated with rituximab. The patients may also subsequently be treated with 177Lu-lilotomab satetraxetan as disclosed herein.
Administration timing
As noted above the radioimmunoconjugates and/or antibody can be used in combination with other types of therapy.
Thus, in a further embodiment of the present invention is the use for a combinational therapy where the radioimmunoconjugate followed by simultaneous or post-treatment with antibody therapy, immunoconjugate therapy or a combination thereof, as described elsewhere herein.
Such therapy or treatment may be a monoclonal antibody selected from rituximab and lilotomab (HH 1) depending on the antigen in focus.
The therapy can be repeated in cyclic pattern where administration of the radioimmunoconjugates and the monoclonal antibodies are repeated once, twice or several times.
A further embodiment of the present invention relates to the predosing of lilotomab done less than 24 hours, such as within 4 hours before administration of 177Lu-lilotomab satetraxetan.
Another embodiment of the present invention relates to the predosing of lilotomab done less than 12 hours before administration of 177Lu-lilotomab satetraxetan.
A further embodiment of the present invention relates to the predosing of lilotomab done less than 8 hours before administration of 177Lu-lilotomab satetraxetan.
Yet another embodiment of the present invention relates to the predosing of lilotomab done less than 4 hours before administration of 177Lu-lilotomab satetraxetan.
A further embodiment of the present invention relates to the predosing of lilotomab done less than 2 hours before administration of 177Lu-lilotomab satetraxetan.
Rituximab administration
Rituximab is a monoclonal antibody against the protein CD20, which is primarily found on the surface of immune system B cells. Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 375 mg/m2 rituximab.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one injection or infusion of 375 mg/m2 rituximab.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with two injections or infusions of 375 mg/m2 rituximab.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with three or more injections or infusions of 375 mg/m2 rituximab.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 100-750 mg/m2 rituximab.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 200-750 mg/m2 rituximab.
Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with one, two, three or more injections or infusions of 300-700 mg/m2 rituximab. Another embodiment of the present invention relates to the uses and methods of the present invention further comprising a pretreatment step before predosing wherein the pretreatment step comprises pretreatment with 375 mg/m2 rituximab. This treatment can be repeated, once, twice or several times. Rituximab can be injected or infused. The pretreatment can be done 28-7 days before administration of 177Lu-lilotomab satetraxetan. Another embodiment of the present invention relates to rituximab infused or injected once or twice 28-14 days before administration of 177Lu-lilotomab satetraxetan. An additional infusion or injection of rituximab can be done less than 4 hours before administration of 177Lu-lilotomab satetraxetan.
Another embodiment of the present invention relates to rituximab infused or injected once or twice 10-18 days before administration of 177Lu-lilotomab satetraxetan.
Another embodiment of the present invention relates to rituximab infused or injected once, twice, or three times at day 28, 21 or 14 before administration of 177l_u-lilotomab satetraxetan.
Yet another embodiment of the present invention relates to 375 mg/m2 rituximab infused or injected at 28 and 21 days before administration of 177l_u-lilotomab satetraxetan.
A further embodiment of the present invention relates to 375 mg/m2 rituximab infused or injected at 14 days before administration of 177Lu-lilotomab satetraxetan. Another embodiment of the present invention relates to 375 mg/m2 rituximab infused or injected at 14 days and again less than 4 hours before administration of 177Lu- lilotomab satetraxetan.
Specific administration patterns
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 40 mg/patient of lilotomab, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.Another aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 40 mg/m2 lilotomab, followed by 17.5 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 60 mg/m2 lilotomab, followed by 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 30 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 35 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 45 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. Another aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of INon-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 17,5 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 20 MBq/kg 177l_u-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising predosing of 100 mg/m2 lilotomab, followed by 30 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days prior to administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days prior to administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab, followed by 17,5 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days prior to administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab, followed by 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days prior to administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab, followed by 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
An aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 1 Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days prior to administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab, followed by 30 MBq/kg 177l_u-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 17,5 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according in an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 30 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. Another aspect of the present invention relates to lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177l_u-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to a combination of lilotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177l_u-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to a combination of lilotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 17,5 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to a combination of lilotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to a combination of lilotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
A further aspect of the present invention relates to a combination of lilotomab and 177Lu- lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177l_u-lilotomab satetraxetan, followed by 30 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Yet another aspect of the present invention relates to lilotomab for use in the reduction of haematological toxicity due to the administration of 177l_u-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 17,5 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
Another aspect of the present invention relates to a method of treating Non-Hodgkin lymphoma comprising administration of pretreatment using 375 mg/m2 rituximab 14 days before administration of 177Lu-lilotomab satetraxetan and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan, predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu-lilotomab satetraxetan, followed by 30 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. The therapy or treatment of the present invention can be administered either as a monotherapy or in combination with other therapies, preferentially standard treatments.
An aspect of the present invention relates to the treatment patterns shown in Arm 1 of figure 8.
An aspect of the present invention relates to the treatment patterns shown in Arm 2 of figure 8. An aspect of the present invention relates to the treatment patterns shown in Arm 3 of figure 8.
An aspect of the present invention relates to the treatment patterns shown in Arm 4 of figure 8.
Pre-medication consisting of an antipyretic and antihistamine medication can be administered before infusion of rituximab. The types of pre-medication are in accordance with each hospital's routine, including any use of corticosteroids.
Pharmaceutical compositions
Antibodies and radioimmunoconjugates are usually applied in the treatment of diseases formulated in pharmaceutical compositions.
Such compositions are optimized for parameters such as physiological tolerance and shelf-life.
Thus, in one embodiment of the present invention is the radioimmunoconjugates and/or antibodies of the present invention formulated as a pharmaceutical composition.
An embodiment of the present invention relates to a pharmaceutical composition as described above, further comprising one or more additional therapeutic agents.
In another embodiment of the present invention are said one or more additional therapeutic agents selected from agents that induce apoptosis.
Usually is an important element of a pharmaceutical composition a buffer solution, which to a substantial degree maintain the chemical integrity of the radioimmunoconjugate and/or antibody and is being physiologically acceptable for infusion into patients.
In one embodiment of the present invention the pharmaceutical composition comprises one or more pharmaceutically acceptable carriers and/or adjuvants.
Acceptable pharmaceutical carriers include but are not limited to non-toxic buffers, fillers, isotonic solutions, etc. More specifically, the pharmaceutical carrier can be but are not limited to normal saline (0.9 %), half-normal saline, Ringer's lactate, 5 % Dextrose, 3.3 % Dextrose/0.3 % Saline. The physiologically acceptable carrier can contain a radiolytic stabilizer, e.g., ascorbic acid, which protect the integrity of the radiopharmaceutical during storage and shipment.
In one embodiment of the present invention are lilotomab and Betalutin formulated as indicated in Tables 1 and 2 in Example 1. Preferably are sodium dihydrogen phosphate monohydrate, sodium chloride, recombinant human albumin, sodium ascorbate, diethylenetriamine pentaacetic acid (DTPA) and sodium hydroxide used as excipients in the formulation buffer.
Preferably is phosphate included in the formulation buffer to maintain the pH of the finished product during the shelf life.
Preferably is recombinant human albumin included in the formulation buffer as a stabilizer for the lilotomab satetraxetan conjugate. The albumin also acts as a radioprotectant. Recombinant human albumin structurally identical to human serum albumin derived from yeast is used. No human- or animal-derived raw material is involved in its manufacture. The excipient is well known and is used in pharmaceutical products for human use.
Preferably is sodium ascorbate included in the formulation to act as a radiolytic scavenger to ensure the stability of Betalutin over the shelf-life of the product.
Preferably is DTPA introduced as an excipient in the Betalutin formulation to chelate any free 177Lu3+ ions and to reroute this impurity from accumulation in the bone to rapid renal clearance (Li et al 2001, Breeman et al 2003). Betalutin contains 9.3 μιτιοΙ DTPA in 12 mL, while the maximum amount of no-carrier added (n.c.a) 177Lu3+ (> 3,000 GBq/mg) applied (6.9 GBq) corresponds to less than 15 nmol Lu ions. This gives a more than 1000-fold molar excess of DTPA over Lu3+ ions. Furthermore, when taking into account that the majority of the Lu3+ ions (> 95%) is chelated to lilotomab satetraxetan, the molar excess is almost 100,000-fold. DTPA is therefore expected to chelate all free 177Lu3+ ions quantitatively and 177Lu-DTPA is thus specified as radiochemical impurity in the specification.
Preferably is the formulation buffer an aqueous solution with pH 6.9 to 7.0 and thus no incompatibilities between the drug substance and the formulation buffer are expected.
One embodiment of the present invention comprises the pharmaceutical composition of the present invention and one or more additional antibodies or radioimmunoconjugates.
As aspect of the present invention relates to a pharmaceutical composition comprising (per mL) : 0.75 mg Lutetium (177Lu) lilotomab satetraxetan, 0.46 mg Ammonium acetate, and Trace amounts of HCb.
Another aspect of the present invention relates to a pharmaceutical composition comprising (per mL): 30.86 mg Sodium ascorbate, 0.31 mg DTPA, 0.17 mg NaOH, 60.82 mg Recombinant human albumin, 3.32 mg Sodium dihydrogen phosphate monohydrate, and 4.34 mg Sodium chloride with the pH is adjusted to 6.9-7.0.
A further aspect of the present invention relates to a pharmaceutical composition comprising;
14% of the pharmaceutical composition comprising (per ml_) : 0.75 mg Lutetium (177Lu) lilotomab satetraxetan, 0.46 mg Ammonium acetate, and Trace amounts of HCI3, and 86% of the pharmaceutical composition comprising (per ml_) : 30.86 mg Sodium ascorbate, 0.31 mg DTPA, 0.17 mg NaOH, 60.82 mg Recombinant human albumin, 3.32 mg Sodium dihydrogen phosphate monohydrate, and 4.34 mg Sodium chloride with the pH is adjusted to 6.9-7.0.
The present invention also relates to the pharmaceutical compositions of the present examples, as well as the dosage administration patterns presented herein. This includes the use of the pharmaceutical compositions of the present invention for use in the treatment of Non-Hodgkin lymphoma.
Cancer types
The person in need of treatment with 177Lu-lilotomab satetraxetan is suffering from a CD37 related disease, typically a B-cell lymphoma such as Non-Hodgkin lymphoma (NHL).
NHL is a group of blood cancers that includes all types of lymphoma except Hodgkin's lymphomas. Symptoms include enlarged lymph nodes, fever, night sweats, weight loss, and feeling tired. Other symptoms may include bone pain, chest pain, or itchiness. Some forms are slow growing while others are fast growing.
There are several types of NHL. Thus, another embodiment of the present invention relates to the lymphoma being a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, Diffuse large B-cell lymphoma, and mantle cell.
In an embodiment of the present invention is the NHL cancer follicular grade I-IIIA. In an embodiment of the present invention is the NHL cancer marginal zone.
In an embodiment of the present invention is the NHL cancer small lymphocytic.
In an embodiment of the present invention is the NHL cancer lymphoplasmacytic. In an embodiment of the present invention is the NHL cancer mantle cell.
In an embodiment of the present invention is the NHL cancer AML.
In an embodiment of the present invention is the NHL cancer CLL. In an embodiment of the present invention is the NHL cancer Diffuse Large B-cell lymphoma (DLBCL).
Some cell types of leukemia also express the CD37 antigen. Thus, another embodiment of the present invention relates to leukemia of the subtypes chronic lymphocytic leukemia and acute myelogen leukemia. More specifically the present invention relates to AML with 11Q23/MLL translocation. Thus, in one embodiment of the present invention is the NHL cancer AML with 11Q23/MLL translocation.
General
It should be understood that any feature and/or aspect discussed above in
connections with the compounds and particles according to the invention apply by analogy to the methods and applications described herein.
The following figures and examples are provided below to illustrate the present invention. They are intended to be illustrative and are not to be construed as limiting in any way.
EXAMPLES
Example 1 - clinical study on 177 Lu-lilotomab satetraxetan
Materials and methods
Betalutin is an antibody-radionuclide-conjugate (ARC) composed of the radioisotope lutetium-177, the linker benzyl-DOTA and the murine anti-CD37 IgGl antibody, lilotomab. The active moiety is the beta particle emitting nuclide 177Lu. Lutetium-177 has physical half-life of 6.7 days. The antibody lilotomab recognises epitopes on the CD37 antigen, which is abundant on the cell surface of tumours of B-cell origin, including NHL. Betalutin is prepared as a solution for intravenous administration. 1 mg/ml lilotomab antibody will be used, between 7 to 20 mg lilotomab antibody per patient. The amount of lutetium (177Lu)-lilotomab satetraxetan injected per patient will depend on dose level and patient's weight; however, the dose is capped for patients who weigh more than 130 kg (patients heavier than 130 kg will receive the dose for a 130 kg patient). Betalutin are supplied in vials containing a ready to use solution.
The investigational medicinal product will be referred to as Betalutin or lutetium (177Lu)- lilotomab satetraxetan in the protocol.
Rituximab (MabThera) is used as pre-treatment. Rituximab, a chimeric anti-CD20 antibody will be used to clear the circulating normal peripheral B-lymphocytes in the blood and in the spleen before administrating CD37 targeting Betalutin. This may secure better access for Betalutin to less accessible compartments such as lymph nodes and larger tumour masses. Rituximab targets CD20 and will not block the binding of Betalutin CD37 on the B-lymphocytes or tumour cells. Betalutin contains a murine monoclonal antibody which has been shown from in vitro analysis to bind to the human Fc-y receptor Ila. While rituximab binds to CD20 it also binds to the Fc-y receptor Ila and if administered just prior to Betalutin may therefore inhibit the binding of Betalutin to this receptor and improve its biodistribution. Arm 3 has therefore been included in the study via a protocol amendment to test the ability of rituximab to improve the biodistribution of Betalutin. This improved biodistribution may reduce the incidence of myleosuppressive adverse events by decreasing the radioactivity in the bone marrow and spleen.
In Phase I arms 1, 2, and Phase II, two intravenous infusions of 375 mg/m2 rituximab have been given, at 28 Days and 21 Days, before administration of Betalutin. In Phase I, arms 3, 4 and 5, one intravenous infusion of 375 mg/m2 rituximab have been given 14 days before, and in arms 3 and 5 an additional intravenous infusion of 375 mg/m2 rituximab will be given within 4 hours before Betalutin administration on Day 0. Premedication consisting of an antipyretic and antihistamine medication should be administered before infusion of rituximab. The types of pre-medication are in accordance with each hospital's routine, including any use of corticosteroids.
Lilotomab is used as pre-dosing. The same antibody, lilotomab, as used in Betalutin, a murine anti-CD37 antibody, is used to block the binding on remaining B-cells, after rituximab treatment, in the lymphoid organs. One intravenous infusion of 40 mg lilotomab in arm 1, and 100 mg/m2 lilotomab in arm 4 and arm 5, is performed within 4 hours before administration of Betalutin (up to a maximum of 2.7m2 for lilotomab in arm 4 and 5). Pre-medication consisting of an antipyretic and antihistamine medication should be administered before infusion of lilotomab.
Betalutin is administered in a dose of 15-20 Mbq/kg. Arm 4 is 15 Mbq/kg.
An example of administration pattern can be seen in figure 4 and the composition components are shown in tables 1 and 2.
Table 1. Composition of Betalutin Solution for Injection
COMPOSITION FOR THE QUANTITY FUNCTION REFERENCE TO COMPONENTS PER ML STANDARDS
Drug substance
Lutetium (177Lu) lilotomab 0.75 mg Drag substance GMP manufactured satetraxetan • Ammonium acetate 0.46 mg pH adjustment Ph. Eur.
HC13 Trace Solvent for 177Lu Ph. Eur. USP
Formulation buffer
Sodium ascorbate 30.86 mg Radiolytic scavenger USP
DTPA 0.31 mg Chelation of free USP
177Lu
NaOH 0.17 mg pH adjustment Ph. Eur./USP-NF
Recombinant human albumin 60.82 mg Stabiliser/ USP/NF
radioprotectant
Sodium dihydrogen 3.32 mg Buffer USP/BP phosphate monohydrate
Sodium chloride 4.34 mg Osmolyte USP
Table 2. Composition of lilotomab Drug Product
Results
These results are the results of a phase I/II clinical study on humans.
Platelet and neutrophil counts of arm 3 (rituximab predosing) and arm 4 (100 mg/m2 lilotomab predosing) show grade 3-4 toxicity of arm 3 and no toxicity of arm 4 (figures 1 and 2).
The PK profiles show a large separation between the treatment arms. Arm 1= 40 mg lilotomab predosing, Arm 2 = no predosing, Arm 3 = rituximab predosing and Arm 4 = 100 mg/m2 lilotomab predosing (figure 3).
Example 2 - clinical study on 177 Lu-lilotomab satetraxetan
Materials and methods
Materials and methods are the same as in Example 1. In Phase I arms 1, 2, and Phase II, two intravenous infusions of 375 mg/m2 rituximab have been given, at 28 Days and 21 Days, before administration of Betalutin (Figure
5). In Phase I, arms 3 and 4, one intravenous infusion of 375 mg/m2 rituximab have been given 14 days before, and in arm 3 an additional intravenous infusion of 375 mg/m2 rituximab have been given within 4 hours before Betalutin administration on
Day 0 (Figure 5). Pre-medication consisting of an antipyretic and antihistamine medication should be administered before infusion of rituximab. The types of premedication are in accordance with each hospital's routine, including any use of corticosteroids. Lilotomab is used as pre-dosing. The same antibody, lilotomab, as used in Betalutin, a murine anti-CD37 antibody, is used to block the binding on remaining B-cells, after rituximab treatment, in the lymphoid organs. One intravenous infusion of 40 mg lilotomab in arm 1, and 100 mg/m2 lilotomab in arm 4, is performed within 4 hours before administration of Betalutin (up to a maximum of 2.7m2 for lilotomab in arm 4 and 5). Pre-medication consisting of an antipyretic and antihistamine medication should be administered before infusion of lilotomab.
Betalutin is administered in a dose of 15-20 MBq/kg.
Examples of administration patterns can be seen in figure 5 and the composition components are shown in tables 1 and 2 of example 1.
Results
These results are the results of a phase I/II clinical study on humans.
Platelet and neutrophil counts of patients in arm 1 (40 mg predosing), arm 2 (no predosing), arm 3 (rituximab predosing) and arm 4 (100 mg/m2 lilotomab predosing) show grade 3-4 toxicity of arm 2 and 3, less toxicity of arm 1 and no toxicity of arm 4 (figures 5 and 6).
The PK profiles show a large separation between the treatment arms. Arm 1 = 40 mg lilotomab predosing, Arm 2 = no predosing, Arm 3 = rituximab predosing and Arm 4 = 100 mg/m2 lilotomab predosing (figure 7).
The mean values for platelets and neutrophils at nadir for 23 arm 1 patients were lower than the mean values for 3 arm 4 patients (Figure 9). The dose limiting toxicity and number of grade 3 and 4 adverse events were lower for arm 4 than for arm 1 and highest for arm 2 (Figure 10). The efficacy was equal for all arms (Figure 11). Example 3 - Pre-dosing with lilotomab prior to treatment with 177Lu-lilotomab satetraxetan significantly increases the ratio of tumour to red marrow absorbed dose in non-Hodgkin lymphoma patients
Aim : Four different combinations of pre-dosing and pre-treatment have been investigated. All patients were pre-treated with different regimens of rituximab. Two arms included cold lilotomab pre-dosing (arm 1 and 4; 40 mg fixed and 100 mg/m2 Body Surface Area dosage, respectively) and two did not (arm 2 and 3). Patients received either 10, 15 or 20 MBq 177Lu-lilotomab satetraxetan per kg body weight. Previously, we have shown that absorbed red marrow (RM) doses were lower in arml vs arm2, and that haematological toxicity was more severe for patients receiving higher RM doses. The aim of this work was to compare the ratios of tumour to RM absorbed doses between arm 1, 4 and non-pre-dosed patients (arm 2 + 3).
Materials and Methods: A total of 16 patients were included for RM dosimetry, of these were 14 included for tumour dosimetry. A total of 35 tumours were included, 1 to 5 from each patient (mode 3). RM and mean tumour absorbed doses per administered activity were determined from multiple SPECT/CT-images for each patient. Two-sided student-t- tests were used for all statistical analyses. Results:
The mean RM absorbed doses were 0.83, 0.91 and 1.39 mGy/MBq for arm 1, 4 and non-pre-dosing respectively. There was a significantly higher RM dose for non-pre- dosing compared to arm 1 (p = 0.04), and arm 4 (p = 0.05). Mean tumour absorbed doses were 1.62, 2.78 and 1.37 mGy/MBq for arm 1, 4 and non-pre-dosing
respectively. Tumour doses were higher in arm 4 patients compared to patients without pre-dosing (p = 0.04). Tumour doses in arm 1 were not significantly higher compared to non-pre-dosing (p = 0.71). The mean tumour to RM absorbed dose ratios were 2.16, 3.93 and 1.07 for arm 1, 4 and non-pre-dosing respectively. Ratios were significantly higher in both arm 1 and 4 compared to non-pre-dosing (p = 0.05 and p = 0.04). No statistically significant difference between arm 1 and 4 was found for any parameters (p > = 0.12).
Conclusion :
Pre-dosing with lilotomab has a mitigating effect on red marrow absorbed dose for 177Lu- lilotomab satetraxetan patients, and increased amounts was found correlated with a higher tumour dose. Both pre-dosage levels significantly increased the tumour to RM absorbed dose ratio.
Example 4 - Efficacy and hematological toxicity of 177Lu-lilotomab satetraxetan in non- Hodgkin lymphoma patients
Aim :
Four different combinations of pre-dosing and pre-treatment have been investigated. All patients were pre-treated with different regimens of 375 mg/m2 rituximab. The patients were enrolled into four dose-escalation arms: - Arm 1 : 177Lu-lilotomab satetraxetan + pre-dosing with 40 mg lilotomab (cold anti-CD37 Ab)
Arm 2 : 177Lu-lilotomab satetraxetan without pre-dosing
Arm 3 : 177Lu-lilotomab satetraxetan + pre-dosing with 375 mg/m2 rituximab
Arm 4: 177Lu-lilotomab satetraxetan + pre-dosing with 100 mg/m2 lilotomab Patients received either 10, 15 or 20 MBq 177Lu-lilotomab satetraxetan per kg body weight. The aim of this work was to determine the therapeutic efficacy and
hematological toxicity of each study arm.
After finding the maximum tolerable dose (MTD), arm 1 was continued into a phase 2 part to evaluate efficacy in a larger data-set. Patients and Methods:
The key eligibility criteria was: 1) Age >18 with histologically confirmed relapsed indolent B-cell NHL (follicular grade I-IIIA, mantle cell, SLL, marginal zone,
lymphoplasmacytic subtypes). 2)<25% bone marrow involvement. 3) Life expectancy >3 months. 4) Platelet count > 150 x 109/L. 5) ANC >1.5 x 109/L. 6) No previous hematopoietic stem cell transplantation. Dose-limiting toxicities (DLTs) were assessed during the first 12 weeks. Incidence and severity of adverse events (AEs) according to common terminology criteria for adverse events (CTCAE) v4.0. Response assessments were conducted at 3, 6 (FDG PET-CT), 9, 12, 18, 24 and 36 months (CT) per the International Working Group (IWG) criteria for NHL.
A total of 52 patients were included in the different arms and dose groups according to Table 1.
Table 1. Distribution of patients in different study arms and dose groups
Safety
Overall, 177Lu-lilotomab satetraxetan was well-tolerated. The most common grade 3/4 adverse events were reversible thrombocytopenia and neutropenia. No grade 4 neutropenia/thrombocytopenia was observed with higher lilotomab pre-dosing and 100 mg/m2 gave a higher bone marrow protection than 40 mg (Figs. 1, 2). Dose-limiting toxicities were prolonged but reversible neutropenia and thrombocytopenia (8 patients), and hematuria associated with thrombocytopenia ( 1 patient). The recommended dose for phase 2 expansion of 177Lu-lilotomab satetraxetan in Arm 1 with a lilotomab pre- dose of 40 mg was 15 MBq/kg. Twenty-three patients were included in the current analysis (Table 1, arm 1, 15 MBq/kg). Arm 4, 20 MBq/kg was also selected for expansion into phase 2, but no patients have been included yet. SAEs occurred in 15 patients (25%). Treatment-emergent SAEs occurring in 2 or more patients were thrombocytopenia (n=2), atrial fibrillation (n=2), and lymphoma progression (n=2). Eighteen months after subsequent treatment with bendamustine (24 months after Betalutin®), myelodysplastic syndrome (MDS) or acute myelogen leukemia (AML) was reported in 1 patient with prior alkylating agent exposure. There were no treatment- related deaths. Mean platelet count in Arms 1 and 4 for 15 and 20 MBq/kg 177Lu- lilotomab satetraxetan can be seen in figure 13 and mean neutrophil count in Arms 1 and 4 for 15 and 20 MBq/kg 177Lu-lilotomab satetraxetan can be seen in figure 14.
Efficacy Overall, objective responses were observed in 33 of 52 (63%) patients. 13 patients (25%) achieved a CR (Table 2). Significant activity was seen in patients with relapsed follicular lymphoma (FL) (ORR 70%; CR 24%). The ORR of arm 1, 2 and 3 were similar, while the ORR of arm 4 was lower. There was, however, too few patients in arm 2, 3 and 4 to draw any firm conclusions.
Table 2. Overall response rate (ORR), complete response (CR), partial response (PR), stable disease (SD) and progressive disease (PD) of patients treated with 177Lu- lilotomab satetraxetan
Conclusion :
The hematological toxicity was reduced by pre-dosing with lilotomab.
ITEMS
1. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20-250 mg/m2 lilotomab, followed by
b) 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
2. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to item 1, wherein 177l_u-lilotomab satetraxetan is administered at a concentration selected from the group consisting of 10, 12,5, 15, 17,5, 20, 25, 30, 35, 40, 45 and 50 MBq/kg.
3. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-2, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 15 MBq/kg. 4. 177l_u-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-3, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 17,5 MBq/kg.
5. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-4, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 20 MBq/kg.
6. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-5, wherein lilotomab is administered at a concentration selected from the group consisting of 20 mg/m2, 40 mg/m2, 50 mg/m2, 60 mg/m2, 75 mg/m2, 100 mg/m2, 125 mg/m2, 150 mg/m2, 200 mg/m2, 250 mg/m2, 20 mg/patient and 40 mg/patient.
7. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-6, wherein lilotomab is administered at 20 mg/m2. 8. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-7, wherein lilotomab is administered at 40 mg/m2.
9. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-8, wherein lilotomab is administered at 60 mg/m2.
10. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-8, wherein lilotomab is administered at 100 mg/m2. 11. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-9, wherein lilotomab is administered at 20 mg/patient.
12. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-9, wherein lilotomab is administered at 40 mg/patient.
13. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-12, wherein the predosing of lilotomab is done less than 24 hours, such as within 4 hours before administration of 177Lu-lilotomab satetraxetan. 14. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-13, further comprising a pretreatment step before step a), wherein the pretreatment step comprises pretreatment with one, two, three or more administrations of 375 mg/m2 rituximab. 15. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to item 14, wherein 375 mg/m2 rituximab is administered at 28 and 21 days before administration of 177Lu-lilotomab satetraxetan.
16. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to item 14, wherein 375 mg/m2 rituximab is administered at 14 days before administration of 177Lu-lilotomab satetraxetan.
17. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to items 14 and 16, wherein 375 mg/m2 rituximab is infused at 14 days before and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan. 18. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-17, wherein the lymphoma is a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, AML, CLL, BLBCL, AML with 11Q23/MLL translocation, and mantle cell.
19. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of items 1-12, wherein the patient is relapsing after treatment with rituximab.
20. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20-250 mg/m2 lilotomab, followed by
b) 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
21. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20-100 mg/m2 lilotomab, followed by
b) 10-20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
22. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to item 20-21, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 10 MBq/kg.
23. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to item 20-21, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 15 MBq/kg. 24. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-20, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 17,5 MBq/kg. 25. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein 177Lu-lilotomab satetraxetan is 3administered at a concentration 20 MBq/kg.
26. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 20 mg/m2.
27. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 40 mg/m2.
28. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 60 mg/m2. 29. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 100 mg/m2.
30. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 20 mg/patient.
31. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 40 mg/patient.
31. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 60 mg/kg. 31. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to items 20-21, wherein lilotomab is administered at 100 mg/kg.
33. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 40 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
34. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 40 mg/patient lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
35. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 100 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 36. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 60 mg/m2 lilotomab, followed by
b) 10 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
37. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 60 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
38. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 60 mg/m2 lilotomab, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
39. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20 mg/patient lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 40. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20 mg/patient lilotomab, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
41. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
42. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 100 mg/m2 lilotomab, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 43. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20-250 mg/m2 lilotomab, followed by
b) 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
44. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 43, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 10 MBq/kg. 45. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 43, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 15 MBq/kg.
46. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 43, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 17,5
MBq/kg.
47. A combination of lilotomab and 177l_u-lilotomab satetraxetan for use according to item 43, wherein 177Lu-lilotomab satetraxetan is administered at a concentration 20 MBq/kg.
48. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 36, wherein lilotomab is administered at 20 mg/m2. 49. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 36, wherein lilotomab is administered at 40 mg/m2.
50. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 36, wherein lilotomab is administered at 40 mg/patient.
51. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item 36, wherein lilotomab is administered at 100 mg/m2. 52. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use according to item36, wherein lilotomab is administered at 20 mg/patient. 53. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 40 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
54. A combination of lilotomab and 1 7Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 40 mg/patient lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
55. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 100 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
56. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 100 mg/m2 lilotomab, followed by b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 57. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 20-250 mg/m2.
58. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/m2.
59. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
60. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2.
61. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to item 57, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 60 mg/m2. 62. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to items 57-61, wherein "''Lu- lilotomab satetraxetan is administered in a dose of 15 MBq/kg.
63. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to items 57-61, wherein ^Lu- lilotomab satetraxetan is administered in a dose of 17,5 MBq/kg.
64. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan according to items 57-61, wherein 177Lu- lilotomab satetraxetan is administered in a dose of 20 MBq/kg. 65. Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/m2. 66. Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
67. Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2.
68. Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2.
69. Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
70. Lilotomab for use in the reduction of haematological toxicity due to the administration of 17,5 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/patient. 71. Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 40 mg/patient.
72. Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2.
73. Lilotomab for use in the reduction of haematological toxicity due to the administration of 17,5 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2. 74. Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177l_u-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 100 mg/m2. 75. Lilotomab for use in the reduction of haematological toxicity due to the administration of 10 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 60 mg/m2.
76. Lilotomab for use in the reduction of haematological toxicity due to the administration of 15 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 60 mg/m2.
77. Lilotomab for use in the reduction of haematological toxicity due to the administration of 20 MBq/kg 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 60 mg/m2.
78. A method of treating Non-Hodgkin lymphoma comprising administration of 177Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 20-250 mg/m2 lilotomab, followed by
b) 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 79. A method of treating Non-Hodgkin lymphoma comprising administration of 177Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 20-500 mg/m2 lilotomab, followed by
b) 10-50 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
80. A method of treating Non-Hodgkin lymphoma comprising administration of 177Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 40 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
81. A method of treating Non-Hodgkin lymphoma comprising administration of 177Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 40 mg/patient lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
80. A method of treating Non-Hodgkin lymphoma comprising administration of 177Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 100 mg/m2 lilotomab, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 83. A method of treating Non-Hodgkin lymphoma comprising administration of 177Lu- lilotomab satetraxetan in an administration pattern comprising : a) predosing of 100 mg/m2 lilotomab, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
84. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
85. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 86. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 25 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
87. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 30 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 88. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 60 mg/m2 lilotomab less than 4 hours before administration of ^Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
89. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 60 mg/m2 lilotomab less than 4 hours before administration of ^Lu- lilotomab satetraxetan, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
90. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 40 mg/m2 lilotomab less than 4 hours before administration of ^Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof. 91. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 40 mg/patient lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
92. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 40 mg/patient lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.

Claims

1. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to a clinically relevant administration pattern comprising :
10-20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
2. The 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to claim 1, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20-100 mg/m2 lilotomab, followed by
b) 10-20 MBq/kg 177l_u-lilotomab satetraxetan to a person in need thereof.
3. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 1-2, wherein 177Lu-lilotomab satetraxetan is administered at a concentration of 15 MBq/kg.
4. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to claim 1-3, wherein 177Lu-lilotomab satetraxetan is administered at a concentration of 20 MBq/kg.
5. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 2-4, wherein lilotomab is administered at 20 mg/m2.
6. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 2-4, wherein lilotomab is administered at 60 mg/m2.
7. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 2-4, wherein lilotomab is administered at 100 mg/m2.
8. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 2-4, wherein lilotomab is administered at 40 mg/patient.
9. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 2-8, wherein the predosing of lilotomab is done less than 24 hours before administration of 177Lu-lilotomab satetraxetan.
10. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 1-19, further comprising a pretreatment step before step a), wherein the pretreatment step comprises pretreatment with one, two, three or more administrations of 375 mg/m2 rituximab.
11. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to claim 10, wherein 375 mg/m2 rituximab is administered at 28 and 21 days before administration of 177Lu-lilotomab satetraxetan.
12. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to claim 10, wherein 375 mg/m2 rituximab is administered at 14 days before administration of 177Lu-lilotomab satetraxetan.
13. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to claims 10 or 12, wherein 375 mg/m2 rituximab is infused at 14 days before and again less than 4 hours before administration of 177Lu-lilotomab satetraxetan.
14. 177l_u-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 1-13, wherein the lymphoma is a subtype selected from the group consisting of follicular grade I-IIIA, marginal zone, small lymphocytic, lymphoplasmacytic, AML, CLL, Diffuse large B-cell lymphoma, AML with 11Q23/MLL translocation, and mantle cell.
15. 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma according to any one of claims 1-14, wherein the patient is relapsing after treatment with rituximab.
16. Lilotomab for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab is administered according to an administration pattern comprising : a) predosing of 20-100 mg/m2 lilotomab, followed by
b) 10-20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
17. A combination of lilotomab and 177Lu-lilotomab satetraxetan for use in the treatment of Non-Hodgkin lymphoma wherein lilotomab and 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : a) predosing of 20-100 mg/m2 lilotomab, followed by
b) 10-20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
18. Lilotomab for use in the reduction of haematological toxicity due to the administration of 177Lu-lilotomab satetraxetan, wherein lilotomab is administered before 177Lu-lilotomab satetraxetan in a dose of 20-100 mg/m2.
19. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 100 mg/m2 lilotomab less than 4 hours before administration of ^Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
20. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 100 mg/m2 lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
21. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 60 mg/m2 lilotomab less than 4 hours before administration of ^Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
22. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 60 mg/m2 lilotomab less than 4 hours before administration of ^Lu- lilotomab satetraxetan, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
23. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising : 0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 40 mg/patient lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 15 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
24. 177Lu-lilotomab satetraxetan for use the treatment of Non-Hodgkin lymphoma, wherein 177Lu-lilotomab satetraxetan is administered according to an administration pattern comprising :
0) pretreatment with 375 mg/m2 rituximab administered at 14 days before administration of 177Lu-lilotomab satetraxetan,
a) predosing of 40 mg/patient lilotomab less than 4 hours before administration of 177Lu- lilotomab satetraxetan, followed by
b) 20 MBq/kg 177Lu-lilotomab satetraxetan to a person in need thereof.
25. A pharmaceutical composition comprising (per mL); 0.75 mg Lutetium (177Lu) lilotomab satetraxetan, 0.46 mg Ammonium acetate, and Trace amounts of HCb.
26. A pharmaceutical composition comprising (per mL); 30.86 mg Sodium ascorbate, 0.31 mg DTPA, 0.17 mg NaOH, 60.82 mg Recombinant human albumin, 3.32 mg Sodium dihydrogen phosphate monohydrate, and 4.34 mg Sodium chloride with the pH is adjusted to 6.9-7.0. 27. A pharmaceutical composition comprising; 14% of the pharmaceutical composition according to claim 25 and 86% of the pharmaceutical composition according to claim 26.
27. A pharmaceutical composition comprising (per mL) : 5 mg Lilotomab, 12.7 mg Disodium hydrogen phosphate dodecahydrate, 0.7 mg Sodium dihydrogen phosphate dihydrate, 0.5 mg Sodium chloride, 50 mg Sucrose, 0.2 mg Polysorbate 20, and water for injection ad 1 mL.
28. A pharmaceutical composition according to anyone of claims 25-27, for use in the treatment of Non-Hodgkin lymphoma.
EP17768448.7A 2016-09-16 2017-09-15 Treatment of non-hodgkin lymphoma using lilotomab and 177lu-lilotomab satetraxetan Pending EP3512881A1 (en)

Applications Claiming Priority (5)

Application Number Priority Date Filing Date Title
EP16189191 2016-09-16
EP17164164 2017-03-31
EP17170641 2017-05-11
EP17175768 2017-06-13
PCT/EP2017/073336 WO2018050851A1 (en) 2016-09-16 2017-09-15 Treatment of non-hodgkin lymphoma using lilotomab and 177lu-lilotomab satetraxetan

Publications (1)

Publication Number Publication Date
EP3512881A1 true EP3512881A1 (en) 2019-07-24

Family

ID=59895313

Family Applications (1)

Application Number Title Priority Date Filing Date
EP17768448.7A Pending EP3512881A1 (en) 2016-09-16 2017-09-15 Treatment of non-hodgkin lymphoma using lilotomab and 177lu-lilotomab satetraxetan

Country Status (14)

Country Link
US (2) US20190192703A1 (en)
EP (1) EP3512881A1 (en)
JP (1) JP2019529433A (en)
KR (1) KR20190054113A (en)
CN (1) CN109790219A (en)
AU (1) AU2017327772A1 (en)
BR (1) BR112019004838A2 (en)
CA (1) CA3035268A1 (en)
IL (1) IL265387A (en)
MX (1) MX2019003029A (en)
PH (1) PH12019550033A1 (en)
RU (1) RU2019110955A (en)
SG (2) SG11201901672RA (en)
WO (1) WO2018050851A1 (en)

Families Citing this family (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
KR20200036913A (en) 2017-08-04 2020-04-07 브리스톨-마이어스 스큅 컴퍼니 [1,2,4] triazolo [4,3-a] pyridinyl substituted indole compounds
EP3713607A1 (en) * 2017-11-22 2020-09-30 Nordic Nanovector ASA Radioimmunoconjugates in combination with other drugs as treatment against nhl

Family Cites Families (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JP2003513012A (en) * 1999-08-11 2003-04-08 アイデック ファーマスーティカルズ コーポレイション Treatment of patients with non-Hodgkin's lymphoma with bone marrow lesions by anti-CD20 antibodies
NO331080B1 (en) * 2010-01-29 2011-09-26 Nordic Nanovector As Radioimmune conjugates, pharmaceutical compositions and kits comprising the same and their use
RU2658438C2 (en) * 2011-12-13 2018-06-21 Нордик Нановектор Аса Chimeric therapeutic anti-cd-37 antibody hh1
JP6784687B2 (en) * 2015-02-24 2020-11-11 ザ リージェンツ オブ ザ ユニバーシティ オブ カリフォルニア Binding-induced transcription switch and how to use it

Also Published As

Publication number Publication date
KR20190054113A (en) 2019-05-21
AU2017327772A1 (en) 2019-03-21
US20220160907A1 (en) 2022-05-26
SG11201901672RA (en) 2019-03-28
RU2019110955A3 (en) 2020-11-26
SG10202102588QA (en) 2021-04-29
PH12019550033A1 (en) 2019-07-29
US20190192703A1 (en) 2019-06-27
WO2018050851A1 (en) 2018-03-22
MX2019003029A (en) 2019-09-13
BR112019004838A2 (en) 2019-06-04
RU2019110955A (en) 2020-10-20
CN109790219A (en) 2019-05-21
JP2019529433A (en) 2019-10-17
IL265387A (en) 2019-05-30
CA3035268A1 (en) 2018-03-22

Similar Documents

Publication Publication Date Title
Frantellizzi et al. Targeted alpha therapy with thorium-227
US20220160907A1 (en) Treatment of non-hodgkin lymphoma using lilotomab and 177lu-lilotomab satetraxetan
JP5468597B2 (en) PHARMACEUTICAL COMPOSITION, COMPOSITION, PREPARATION METHOD THEREOF, AND KIT USING THORIUM-227
RU2770073C2 (en) Radiotherapeutic particles and suspensions
Rao et al. Radioimmunotherapy for non-Hodgkin’s lymphoma
Sartor et al. Targeted use of alpha particles: current status in cancer therapeutics
Abbas et al. Preclinical evaluation of 227Th-labeled and 177Lu-labeled trastuzumab in mice with HER-2-positive ovarian cancer xenografts
Kotzerke et al. Radioimmunotherapy for the intensification of conditioning before stem cell transplantation: differences in dosimetry and biokinetics of 188Re-and 99mTc-labeled anti-NCA-95 MAbs
Grudzinski et al. CLR 125 Auger electrons for the targeted radiotherapy of triple-negative breast cancer
US20060228297A1 (en) Thorium-227 for use in radiotherapy of soft tissue disease
Michel et al. 177Lu-antibody conjugates for single-cell kill of B-lymphoma cells in vitro and for therapy of micrometastases in vivo
Lindén et al. A novel platform for radioimmunotherapy: extracorporeal depletion of biotinylated and 90Y-labeled rituximab in patients with refractory B-cell lymphoma
Koenecke et al. Radioimmunotherapy with [188 Re]-labelled anti-CD66 antibody in the conditioning for allogeneic stem cell transplantation for high-risk acute myeloid leukemia
Bailly et al. Radioimmunotherapy of lymphomas
Sowa Dumond et al. Concepts and issues for therapeutic radiopharmaceuticals
Rathmann Development of a Versatile Platform for Combination Targeted Radionuclide and Immune Cell Recruitment Therapies Using Bio-Orthogonal Chemistry
Jadvar Sequential and Combination Therapies of 223 RaCl2 and Prostate-Specific Membrane Antigen Radioligand Therapy
Sgouros et al. MIRD Pamphlet No. 22-Radiobiology and Dosimetry of Alpha-Particle Emitters for Targeted Radionuclide Therapy
Ivanov et al. New insights into the mechanisms of action of radioimmunotherapy in lymphoma
Rathmann et al. CHAPTER FIVE: COMBINED RADIONUCLIDE THERAPY AND IMMUNOTHERAPY FOR TREATMENT OF TRIPLE NEGATIVE BREAST CANCER Preamble
Pagel et al. Radioimmunotherapy and Hematopoietic Cell Transplantation
Sartor et al. Nuclear Medicine & Radiation Therapy
Abbas Comparison of High-and Low-LET radioimmunotherapy in HER-2 positive carcinomas
Abi-Ghanem Radionuclide Therapy of Leukemias
Gopal Radioimmunotherapy of Lymphomas

Legal Events

Date Code Title Description
STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: UNKNOWN

STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: THE INTERNATIONAL PUBLICATION HAS BEEN MADE

PUAI Public reference made under article 153(3) epc to a published international application that has entered the european phase

Free format text: ORIGINAL CODE: 0009012

STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: REQUEST FOR EXAMINATION WAS MADE

17P Request for examination filed

Effective date: 20190315

AK Designated contracting states

Kind code of ref document: A1

Designated state(s): AL AT BE BG CH CY CZ DE DK EE ES FI FR GB GR HR HU IE IS IT LI LT LU LV MC MK MT NL NO PL PT RO RS SE SI SK SM TR

AX Request for extension of the european patent

Extension state: BA ME

DAV Request for validation of the european patent (deleted)
DAX Request for extension of the european patent (deleted)
REG Reference to a national code

Ref country code: HK

Ref legal event code: DE

Ref document number: 40011952

Country of ref document: HK

STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: EXAMINATION IS IN PROGRESS

STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: EXAMINATION IS IN PROGRESS

17Q First examination report despatched

Effective date: 20210118

STAA Information on the status of an ep patent application or granted ep patent

Free format text: STATUS: EXAMINATION IS IN PROGRESS